Your search keyword '"Philip S Portoghese"' showing total 243 results

1. FBNTI, a DOR-Selective Antagonist That Allosterically Activates MOR within a MOR–DOR Heteromer

Author

Philip S. Portoghese, George L. Wilcox, Daniel J. Bruce, Michael Ansonoff, Defeng Tian, Eyup Akgün, Mary M. Lunzer, John E. Pintar, and Jon E. Hawkinson

Subjects

Male, Agonist, medicine.drug_class, Allosteric regulation, Receptors, Opioid, mu, Heteromer, Pharmacology, Biochemistry, Mice, Receptors, Opioid, delta, mental disorders, polycyclic compounds, medicine, Animals, Humans, Receptor, Injections, Spinal, Mice, Knockout, Mice, Inbred ICR, Molecular Structure, Chemistry, HEK 293 cells, Antagonist, Analgesics, Opioid, HEK293 Cells, nervous system, Opioid, Knockout mouse, Calcium, human activities, medicine.drug

Abstract

This report describes the unique pharmacological profile of FBNTI, a potent DOR antagonist that acts as a MOR agonist via an allosteric mechanism. Binding of FBNTI to opioid receptors expressed in HEK 293 cells revealed a 190-fold greater affinity for DOR (Ki = 0.84 nM) over MOR (Ki = 160 nM). In mice, intrathecal FBNTI produced potent antinociception (ED50 = 46.9 pmol/mouse), which was antagonized by selective MOR antagonists (CTOP, β-FNA). Autoantagonism of the MOR agonism by FBNTI was observed above the ED75 dose, suggesting antagonism of activated MOR. That FBNTI is devoid of agonism in DOR knockout mice is consistent with allosteric activation of the MOR protomer via FBNTI bound to within a MOR-DOR heteromer. This proposed mechanism is supported by calcium mobilization assays, which indicate that FBNTI selectively activates the MOR-DOR heteromer and functionally antagonizes the MOR protomer at >ED75. The unprecedented mode of MOR activation by FBNTI may be responsible for the lack of tolerance after intrathecal (i.t.) administration. FBNTI was highly effective upon topical administration to the ipsolateral hind paw in the Hargreaves assay (EC50 = 0.17 ± 0.08 μM) and without significant contralateral activity, suggesting a lack of systemic exposure.

Published

2020

2. Opioid receptors in GtoPdb v.2021.3

Author

Eric J. Simon, Nurulain T. Zaveri, Dominique Massot, Brian M. Cox, Lawrence Toll, Lakshmi A. Devi, Toni S. Shippenberg, Eamonn Kelly, John R. Traynor, Philip S. Portoghese, Mary Jeanne Kreek, Brigitte L. Kieffer, Hiroshi Ueda, Andreas Zimmer, Volker Höllt, Graeme Henderson, Charles Chavkin, Stephen M. Husbands, MacDonald J. Christie, Michael R. Bruchas, Mark Connor, Ian Kitchen, Girolamo Calò, Anna Borsodi, Stefan Schulz, Olivier Civelli, Jean-Claude Meunier, Lee-Yuan Liu-Chen, Yung Hou Wong, and Christopher J. Evans

Subjects

chemistry.chemical_compound, Nociceptin receptor, chemistry, Enkephalin, Opioid, Dynorphin B, medicine, Dynorphin A, (+)-Naloxone, Pharmacology, Receptor, Big dynorphin, medicine.drug

Abstract

Opioid and opioid-like receptors are activated by a variety of endogenous peptides including [Met]enkephalin (met), [Leu]enkephalin (leu), β-endorphin (β-end), α-neodynorphin, dynorphin A (dynA), dynorphin B (dynB), big dynorphin (Big dyn), nociceptin/orphanin FQ (N/OFQ); endomorphin-1 and endomorphin-2 are also potential endogenous peptides. The Greek letter nomenclature for the opioid receptors, μ, δ and κ, is well established, and NC-IUPHAR considers this nomenclature appropriate, along with the symbols spelled out (mu, delta, and kappa), and the acronyms, MOP, DOP, and KOP. [121, 100, 91]. The human N/OFQ receptor, NOP, is considered 'opioid-related' rather than opioid because, while it exhibits a high degree of structural homology with the conventional opioid receptors [294], it displays a distinct pharmacology. Currently there are numerous clinically used drugs, such as morphine and many other opioid analgesics, as well as antagonists such as naloxone, however only for the μ receptor.

Published

2021

3. Combined Glia Inhibition and Opioid Receptor Agonism Afford Highly Potent Analgesics without Tolerance

Author

Eyup Akgün, Mary M. Lunzer, and Philip S. Portoghese

Subjects

Male, Physiology, medicine.drug_class, Cognitive Neuroscience, Pain, Pharmacology, Biochemistry, Mice, 03 medical and health sciences, 0302 clinical medicine, Piperidines, Opioid receptor, medicine, Animals, Receptor, Pain Measurement, 030304 developmental biology, Mice, Inbred ICR, 0303 health sciences, Microglia, Chemistry, Antagonist, Drug Tolerance, Cell Biology, General Medicine, Isoquinolines, Analgesics, Opioid, medicine.anatomical_structure, Receptors, Opioid, Hyperalgesia, NMDA receptor, medicine.symptom, μ-opioid receptor, Neuroglia, 030217 neurology & neurosurgery, Astrocyte

Abstract

Commonly prescribed opioid analgesics produce tolerance upon chronic use due in part to induction of hyperalgesia. Given that two reported bivalent ligands (MMG22 and MCC22) produce potent antinociception without tolerance only in inflamed mice, we have investigated the possible cellular and receptor targets of these ligands. The selective microglia inhibitors, minocycline and SB290157, antagonized intrathecal (i.t.) MCC22 antinociception orders of magnitude more potently than MMG22, suggesting that MCC22 selectively targets activated microglia. The astrocyte toxin, l-α-aminoadipic acid antagonized MMG22 antinociception 126-fold without reducing the potency of MCC22, indicating that activated astrocytes are targets of MMG22. MK-801 and Ro25-6981 antagonism of MMG22 antinociception, but not MCC22, is consistent with selective inhibition of activated NMDAR in astrocytes. The antinociception produced by i.t. MMG22 or MCC22 were both antagonized by the selective mu opioid receptor antagonist, β-FNA, implicating interaction of these ligands with MOR in spinal afferent neurons. MCC22 antinociception was potently blocked by kainate or AMPA ion channel antagonists (LY382884; NBQX), in contrast to MMG22. It is concluded that i.t. MMG22 and MCC22 produce exceptional antinociception via potent inhibition of activated spinal glia, thereby leading to desensitization of spinal neurons and enhanced activation of neuronal MOR. Thus, the present study suggests a new approach to treatment of chronic inflammatory pain without tolerance through a single molecular entity that simultaneously inhibits activated glia and stimulates MOR in spinal neurons.

Published

2018

4. Bivalent ligand that activates mu opioid receptor and antagonizes mGluR5 receptor reduces neuropathic pain in mice

Author

Maureen S. Riedl, Eyup Akgün, Mary M. Lunzer, Carolyn A. Fairbanks, George L. Wilcox, Lucy Vulchanova, Cristina D. Peterson, Philip S. Portoghese, and Kelley F. Kitto

Subjects

Male, 0301 basic medicine, Agonist, medicine.drug_class, Narcotic Antagonists, Receptor, Metabotropic Glutamate 5, Receptors, Opioid, mu, Pharmacology, Ligands, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, mental disorders, medicine, Enzyme-linked receptor, Animals, Injections, Spinal, Analgesics, Chemistry, Metabotropic glutamate receptor 5, 030104 developmental biology, Anesthesiology and Pain Medicine, nervous system, Neurology, Opioid, Hyperalgesia, Oxymorphone, Anesthesia, Neuropathic pain, Neuralgia, Neurology (clinical), medicine.symptom, μ-opioid receptor, 030217 neurology & neurosurgery, medicine.drug

Abstract

The mu opioid receptor (MOR) and metabotropic glutamate receptor 5 (mGluR5) are well-established pharmacological targets in the management of chronic pain. Both receptors are expressed in the spinal cord. MMG22, a bivalent ligand containing 2 pharmacophores separated by 22 atoms, which simultaneously activates MOR and antagonizes mGluR5, has been shown to produce potent reversal of tactile hypersensitivity in rodent models of lipopolysaccharide (LPS)-and bone cancer-induced chronic pain. This study assessed whether intrathecal MMG22 also is effective in reducing pain of neuropathic origin. Furthermore, we theorized that MMG22 should reduce hyperalgesia in nerve-injured mice in a manner consistent with a synergistic interaction between MOR and mGluR5. Several weeks after spared nerve injury, tactile hypersensitivity was reversed in mice by the intrathecal injection of MMG22 (0.01-10 nmol) but also by its shorter spacer analog, MMG10, with similar potency. The potencies of the bivalent ligands were 10- to 14-fold higher than those of the compounds upon which the bivalent structure was based, the MOR agonist oxymorphone and the mGluR5 antagonist MPEP. Coadministration of oxymorphone and MPEP demonstrated analgesic synergism, an interaction confirmed by isobolographic analysis. This study indicates that in the spared nerve injury-induced model of neuropathic pain, the 2 pharmacophores of the bivalent ligands MMG22 and MMG10 target MOR and mGluR5 as separate receptor monomers. The observed increase in the potency of MMG22 and MMG10, compared with oxymorphone and MPEP, may reflect the synergistic interaction of the 2 pharmacophores of the bivalent ligand acting at their respective separate receptor monomers.

Published

2017

5. Opioid receptors (version 2019.4) in the IUPHAR/BPS Guide to Pharmacology Database

Author

Brian M. Cox, Eamonn Kelly, Girolamo Calo, Stephen M. Husbands, Mark Connor, Nurulain T. Zaveri, Jean-Claude Meunier, Anna Borsodi, Lee-Yuan Liu-Chen, Volker Höllt, Graeme Henderson, Eric J. Simon, Toni S. Shippenberg, Hiroshi Ueda, Olivier Civelli, Philip S. Portoghese, Mary Jeanne Kreek, Andreas Zimmer, MacDonald J. Christie, Yung Hou Wong, John R. Traynor, Stefan Schulz, Charles Chavkin, Brigitte L. Kieffer, Michael R. Bruchas, Ian Kitchen, Christopher J. Evans, Dominique Massot, Lawrence Toll, and Lakshmi A. Devi

Subjects

chemistry.chemical_compound, Nociceptin receptor, Enkephalin, chemistry, Opioid, Dynorphin B, medicine, Dynorphin A, (+)-Naloxone, Pharmacology, Receptor, Big dynorphin, medicine.drug

Abstract

Opioid and opioid-like receptors are activated by a variety of endogenous peptides including [Met]enkephalin (met), [Leu]enkephalin (leu), β-endorphin (β-end), α-neodynorphin, dynorphin A (dynA), dynorphin B (dynB), big dynorphin (Big dyn), nociceptin/orphanin FQ (N/OFQ); endomorphin-1 and endomorphin-2 are also potential endogenous peptides. The Greek letter nomenclature for the opioid receptors, μ, δ and κ, is well established, and NC-IUPHAR considers this nomenclature appropriate, along with the symbols spelled out (mu, delta, and kappa), and the acronyms, MOP, DOP, and KOP. [116, 96, 88]. The human N/OFQ receptor, NOP, is considered 'opioid-related' rather than opioid because, while it exhibits a high degree of structural homology with the conventional opioid receptors [282], it displays a distinct pharmacology. Currently there are numerous clinically used drugs, such as morphine and many other opioid analgesics, as well as antagonists such as naloxone, however only for the μ receptor.

Published

2019

6. Targeting MOR-mGluR(5) heteromers reduces bone cancer pain by activating MOR and inhibiting mGluR5

Author

Samuel J. Erb, Catherine Harding-Rose, Sarah S. Shueb, Donald A. Simone, Philip S. Portoghese, Rebecca Speltz, Eyup Akgün, and Mary M. Lunzer

Subjects

0301 basic medicine, Agonist, Male, medicine.drug_class, Fibrosarcoma, Receptors, Opioid, mu, Bone Neoplasms, Pharmacology, Ligands, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, Mice, 0302 clinical medicine, Receptors, Kainic Acid, medicine, Animals, Mice, Inbred C3H, Morphine, Bone cancer, business.industry, Drug Administration Routes, Cancer Pain, medicine.disease, Conditioned place preference, Disease Models, Animal, 030104 developmental biology, Mechanism of action, Opioid, Hyperalgesia, Systemic administration, medicine.symptom, Cancer pain, business, 030217 neurology & neurosurgery, medicine.drug

Abstract

Pain is among the most common symptoms in cancer and approximately 90% of patients experience end-stage cancer pain. The management of cancer pain is challenging due to the significant side effects associated with opioids, and novel therapeutic approaches are needed. MMG22 is a bivalent ligand containing MOR agonist and mGluR5 antagonist pharmacophores joined by a 22-atom spacer. MMG22 exhibited extraordinary analgesia following intrathecal administration in a mouse model of bone cancer pain. Here, we assessed the effectiveness of systemic administration of MMG22 in reducing cancer pain and evaluated whether MMG22 displays side effects associated with opioids. Fibrosarcoma cells were injected into and around the calcaneus bone in C3H mice. Mechanical hyperalgesia was defined as an increase in the paw withdrawal frequencies (PWFs) evoked by application of a von Frey monofilament (3.9 mN bending force) applied to the plantar surface of the hind paw Subcutaneous (s.c.), intramuscular (i.m.), and oral (p.o.) administration of MMG22 produced robust dose-dependent antihyperalgesia, whose ED50 was orders of magnitude lower than morphine. Moreover, the ED50 for MMG22 decreased with disease progression. Importantly, s.c. administration of MMG22 did not produce acute (24 h) or long-term (9 days) tolerance, was not rewarding (conditioned place preference test), and did not produce naloxone-induced precipitated withdrawal or alter motor function. A possible mechanism of action of MMG22 is discussed in terms of inhibition of spinal NMDAR via antagonism of its co-receptor, mGluR5, and concomitant activation of neuronal MOR. We suggest that MMG22 may be a powerful alternative to traditional opioids for managing cancer pain. This article is part of the Special Issue entitled ‘New Vistas in Opioid Pharmacology’.

Published

2019

7. Bivalent ligand MCC22 potently attenuates nociception in a murine model of sickle cell disease

Author

Gregory M. Vercellotti, John D. Belcher, Julie K. Olson, Philip S. Portoghese, Donald A. Simone, Eyup Akgün, Mary M. Lunzer, and Giuseppe Cataldo

Subjects

0301 basic medicine, Male, Nociception, congenital, hereditary, and neonatal diseases and abnormalities, Cell, Mice, Transgenic, Disease, Anemia, Sickle Cell, Pharmacology, Bivalent (genetics), Article, 03 medical and health sciences, Mice, 0302 clinical medicine, hemic and lymphatic diseases, medicine, Animals, Analgesics, business.industry, Chronic pain, medicine.disease, Chronic inflammatory disorder, Analgesics, Opioid, Disease Models, Animal, 030104 developmental biology, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Neurology, Murine model, Hyperalgesia, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Sickle cell disease (SCD) is a chronic inflammatory disorder accompanied by chronic pain. In addition to ongoing pain and hyperalgesia, vaso-occlusive crises-induced pain can be chronic or episodic. Since analgesics typically used to treat pain are not very effective in SCD, opioids, including morphine, are a primary treatment for managing pain in SCD but are associated with many serious side effects, including constipation, tolerance, addiction, and respiratory depression. Thus, there is a need for the development of novel treatments for pain in SCD. In this study we used the Townes transgenic mouse model of SCD to investigate the anti-nociceptive efficacy of the bivalent ligand, MCC22, and compared its effectiveness to morphine. MCC22 consists of a mu opioid receptor (MOR) agonist and a chemokine receptor-5 (CCR5) antagonist that are linked through a 22-atom spacer. Our results show that intraperitoneal administration of MCC22 produced exceptionally potent dose-dependent anti-hyperalgesia as compared to morphine, dramatically decreased evoked responses of nociceptive dorsal horn neurons, and decreased expression of pro-inflammatory cytokines in the spinal cord. Moreover, tolerance did not develop to its analgesic effects following repeated administration. In view of the extraordinary potency of MCC22 without tolerance, MCC22 and similar compounds may vastly improve the management of pain associated with SCD.

Published

2018

8. A bivalent compound targeting CCR5 and the mu opioid receptor treats inflammatory arthritis pain in mice without inducing pharmacologic tolerance

Author

Philip S. Portoghese, Eyup Akgün, Bryce A. Binstadt, Mary M. Lunzer, Raini Dutta, and Jennifer L. Auger

Subjects

0301 basic medicine, Agonist, lcsh:Diseases of the musculoskeletal system, Receptors, CCR5, medicine.drug_class, Chemokine receptor, Inflammatory arthritis, Receptors, Opioid, mu, Arthritis, Pain, Mice, Transgenic, Pharmacology, Arthritis, Rheumatoid, 03 medical and health sciences, Mice, 0302 clinical medicine, Piperidines, Drug tolerance, Opioid receptor, Medicine, Animals, Rheumatoid arthritis, Inflammation, Analgesics, business.industry, Drug Tolerance, medicine.disease, Isoquinolines, Arthritis, Experimental, Mice, Inbred C57BL, 030104 developmental biology, Opioid, Heteromer, Morphine, μ-opioid receptor, lcsh:RC925-935, Analgesia, business, CCR5, 030217 neurology & neurosurgery, medicine.drug, Research Article

Abstract

Background Pain accompanies rheumatoid arthritis and other chronic inflammatory conditions and is difficult to manage. Although opioids provide potent analgesia, chronic opioid use can cause tolerance and addiction. Recent studies have demonstrated functional interactions between chemokine and opioid receptor signaling pathways. Reported heterodimerization of chemokine and opioid receptors led our group to develop bivalent compounds that bind both types of receptors, with the goal of targeting opioids to sites of inflammation. MCC22 is a novel bivalent compound containing a CCR5 antagonist and mu opioid receptor (MOR) agonist pharmacophores linked through a 22-atom spacer. We evaluated the efficacy of MCC22 in the K/B.g7 T-cell receptor transgenic mouse model of spontaneous inflammatory arthritis. Methods MCC22 or morphine was administered intraperitoneally at varying doses to arthritic K/B.g7 mice or nonarthritic control mice. Mechanical pain hypersensitivity was measured each day before and after drug administration, using the electronic von Frey test. The potency of MCC22 relative to that of morphine was calculated. Functional readouts of pain included grip strength and nesting behavior. A separate dosing regimen was used to determine whether the drugs induced pharmacologic tolerance. Results MCC22 provided ~ 3000-fold more potent analgesia than morphine in this model. Daily treatment with MCC22 also led to a cumulative analgesic effect, reducing the daily baseline pain level. MCC22 produced no observable analgesic effect in nonarthritic control mice. Importantly, repeated administration of MCC22 did not induce pharmacologic tolerance, whereas a similar regimen of morphine did. Both grip strength and nesting behaviors improved among arthritic mice treated with MCC22. Ankle thickness and arthritis scores were not affected by MCC22. The analgesic effect of MCC22 was abolished in K/B.g7 mice genetically lacking CCR5, demonstrating the receptor specificity of the antagonist pharmacophore. Conclusions MCC22 is a novel bivalent ligand that targets CCR5 and MOR. Our findings demonstrate that MCC22 provides highly potent analgesia and improved functional outcomes in a model of inflammatory arthritis, without inducing typical opioid tolerance. These findings suggest that MCC22 or similar compounds could be used to treat the pain associated with inflammatory arthritis and related conditions, while minimizing the risks typically associated with chronic opioid use. Electronic supplementary material The online version of this article (10.1186/s13075-018-1661-5) contains supplementary material, which is available to authorized users.

Published

2017

9. Heteromer Induction: An Approach to Unique Pharmacology?

Author

Eyup Akgün, Mary M. Lunzer, and Philip S. Portoghese

Subjects

0301 basic medicine, Physiology, medicine.drug_class, Cognitive Neuroscience, Receptor, Metabotropic Glutamate 5, Heteromer, Receptors, Opioid, mu, Plasma protein binding, Pharmacology, Ligands, Biochemistry, Bivalent (genetics), 03 medical and health sciences, Structure-Activity Relationship, 0302 clinical medicine, Opioid receptor, Receptors, Opioid, delta, mental disorders, medicine, Structure–activity relationship, Animals, Humans, Receptor, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Cell Biology, General Medicine, Analgesics, Opioid, 030104 developmental biology, nervous system, Models, Chemical, Pharmacophore, μ-opioid receptor, Protein Multimerization, 030217 neurology & neurosurgery, Protein Binding

Abstract

It is proposed that two types of opioid receptor heteromers exist: a) those that are constitutive and b) those that are induced by bivalent ligands. Mu opioid agonists interact with constitutive MOR-DOR heteromer to mediate tolerance and dependence. Bivalent ligand, MDAN21, is devoid of these adverse effects by virtue of its DOR antagonist pharmacophore. We propose that bivalent ligands MMG22 and MCC22 induce colocalized receptors to form heteromers (MOR-mGluR5 and MOR-CCR5, respectively) that do not occur naturally, thereby promoting unique pharmacology. Heteromer induction with bivalent ligands offers a general approach to unique pharmacology that complements traditional SAR.

Published

2017

10. Targeting putative mu opioid/metabotropic glutamate receptor-5 heteromers produces potent antinociception in a chronic murine bone cancer model

Author

Alvin J. Beitz, Philip S. Portoghese, Branden A. Smeester, Eyup Akgün, and Mary M. Lunzer

Subjects

Male, Nociception, Agonist, medicine.drug_class, Receptor, Metabotropic Glutamate 5, Receptors, Opioid, mu, Heteromer, Pain, Bone Neoplasms, Pharmacology, Ligands, Article, Mice, Drug tolerance, Cell Line, Tumor, mental disorders, medicine, Animals, Analgesics, Mice, Inbred C3H, Morphine, Chemistry, Metabotropic glutamate receptor 5, Chronic pain, Drug Tolerance, medicine.disease, Hyperalgesia, medicine.symptom, μ-opioid receptor

Abstract

The therapeutic management of chronic pain associated with many cancers is problematic due to the development of tolerance and other adverse effects during the disease progression. Recently we reported on a bivalent ligand (MMG22) containing both mu agonist and mGluR5 antagonist pharmacophores that produced potent antinociception in mice with LPS-induced acute inflammatory pain via a putative MOR-mGluR5 heteromer. In the present study we have investigated the antinociception of MMG22 in a mouse model of bone cancer pain to determine its effectiveness in reducing this type of chronic nociception. There was a 572-fold increase in the potency of MMG22 over a period of 3-21 days that correlated with the progressive increase in hyperalgesia induced by bone tumor growth following implantation of fibrosarcoma cells in mice. The enhancement of antinociception with the progression of the cancer is possibly due to inhibition of NMDA receptor-mediated hyperalgesia via antagonism of mGluR5 and concomitant activation of MOR by the MMG22-occupied heteromer. Notably, MMG22 was 3.6-million-fold more potent than morphine at PID 21. Since MMG22 exhibited a 250,000-times greater potency than that of a mixture of the mu opioid (M19) agonist and mGluR5 antagonist (MG20) monovalent ligands, the data suggest that targeting the putative MOR-mGluR5 heteromer is far superior to univalent interaction with receptors in reducing tumor-induced nociception. In view of the high potency, long duration (>24h) of action and minimal side effects, MMG22 has the potential to be a superior pharmacological agent than morphine and other opiates in the treatment of chronic cancer pain and to serve as a novel pharmacologic tool.

Published

2014

11. Putative Kappa Opioid Heteromers As Targets for Developing Analgesics Free of Adverse Effects

Author

Philip S. Portoghese, Michael D. Powers, Mark J. Thomas, Alexander E. Kalyuzhny, Michael A. Benneyworth, Mary M. Lunzer, and Morgan Le Naour

Subjects

Agonist, Indoles, medicine.drug_class, Arrestins, Substance-Related Disorders, Receptors, Opioid, mu, Pharmacology, Naltrexone, Article, 03 medical and health sciences, Mice, Structure-Activity Relationship, 0302 clinical medicine, In vivo, Receptors, Opioid, delta, Drug Discovery, medicine, Avoidance Learning, Animals, Humans, Receptor, beta-Arrestins, 030304 developmental biology, 0303 health sciences, Analgesics, Chemistry, Beta-Arrestins, Receptors, Opioid, kappa, HEK 293 cells, Stereoisomerism, Drug Tolerance, Conditioned place preference, 3. Good health, HEK293 Cells, Opioid, Molecular Medicine, Calcium, Protein Multimerization, 030217 neurology & neurosurgery, medicine.drug

Abstract

It is now generally recognized that upon activation by an agonist, β-arrestin associates with G protein-coupled receptors and acts as a scaffold in creating a diverse signaling network that could lead to adverse effects. As an approach to reducing side effects associated with κ opioid agonists, a series of β-naltrexamides 3-10 was synthesized in an effort to selectively target putative κ opioid heteromers without recruiting β-arrestin upon activation. The most potent derivative 3 (INTA) strongly activated KOR-DOR and KOR-MOR heteromers in HEK293 cells. In vivo studies revealed 3 to produce potent antinociception, which, when taken together with antagonism data, was consistent with the activation of both heteromers. 3 was devoid of tolerance, dependence, and showed no aversive effect in the conditioned place preference assay. As immunofluorescence studies indicated no recruitment of β-arrestin2 to membranes in coexpressed KOR-DOR cells, this study suggests that targeting of specific putative heteromers has the potential to identify leads for analgesics devoid of adverse effects.

Published

2014

12. Ligands that interact with putative MOR-mGluR5 heteromer in mice with inflammatory pain produce potent antinociception

Author

Philip S. Portoghese, Branden A. Smeester, Muhammad I. Javed, Eyup Akgün, Mary M. Lunzer, and Al J Beitz

Subjects

Agonist, medicine.drug_class, Receptor, Metabotropic Glutamate 5, Receptors, Opioid, mu, Heteromer, Pain, Pharmacology, Ligands, Receptors, Metabotropic Glutamate, Mice, medicine, Animals, Inflammation, Multidisciplinary, Metabotropic glutamate receptor 5, Chemistry, Antagonist, Biological Sciences, Analgesics, Opioid, Metabotropic receptor, nervous system, Opioid, Morphine, μ-opioid receptor, Protein Binding, medicine.drug

Abstract

The low effectiveness of morphine and related mu opioid analgesics for the treatment of chronic inflammatory pain is a result of opioid-induced release of proinflammatory cytokines and glutamate that lower the pain threshold. In this regard, the use of opioids with metabotropic glutamate-5 receptor (mGluR 5 ) antagonist has been reported to increase the efficacy of morphine and prevent the establishment of adverse effects during chronic use. Given the presence of opioid receptors (MORs) and mGluR 5 in glia and neurons, together with reports that suggest coexpressed MOR/mGluR 5 receptors in cultured cells associate as a heteromer, the possibility that such a heteromer could be a target in vivo was addressed by the design and synthesis of a series of bivalent ligands that contain mu opioid agonist and mGluR 5 antagonist pharmacophores linked through spacers of varying length (10–24 atoms). The series was evaluated for antinociception using the tail-flick and von Frey assays in mice pretreated with lipopolysaccharide (LPS) or in mice with bone cancer. In LPS-pretreated mice, MMG22 (4c, 22-atom spacer) was the most potent member of the series (intrathecal ED 50 ∼9 fmol per mouse), whereas in untreated mice its ED 50 was more than three orders of magnitude higher. As members of the series with shorter or longer spacers have ≥500-fold higher ED 50s in LPS-treated mice, the exceptional potency of MMG22 may be a result of the optimal bridging of protomers in a putative MOR-mGluR 5 heteromer. The finding that MMG22 possesses a >10 6 therapeutic ratio suggests that it may be an excellent candidate for treatment of chronic, intractable pain via spinal administration.

Published

2013

13. Bivalent Ligands That Target μ Opioid (MOP) and Cannabinoid1 (CB1) Receptors Are Potent Analgesics Devoid of Tolerance

Author

Eyup Akgün, Philip S. Portoghese, Mary M. Lunzer, Mike D. Powers, Alexander E. Kalyuzhny, Morgan Le Naour, and Ajay S. Yekkirala

Subjects

Male, Agonist, Cannabinoid receptor, medicine.drug_class, medicine.medical_treatment, Receptors, Opioid, mu, Heteromer, Fluorescent Antibody Technique, Pain, Pharmacology, Ligands, Article, Structure-Activity Relationship, Receptor, Cannabinoid, CB1, Drug tolerance, mental disorders, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Receptor, Injections, Spinal, Injections, Intraventricular, Mice, Inbred ICR, Molecular Structure, Chemistry, Cell Membrane, Drug Tolerance, Endocytosis, Analgesics, Opioid, HEK293 Cells, Models, Chemical, nervous system, Opioid, Drug Design, Molecular Medicine, lipids (amino acids, peptides, and proteins), Cannabinoid, medicine.drug

Abstract

Given that μ opioid (MOP) and canabinoid (CB1) receptors are colocalized in various regions of the central nervous system and have been reported to associate as heteromer (MOP-CB1) in cultured cells, the possibility of functional, endogenous MOP-CB1 in nociception and other pharmacologic effects has been raised. As a first step in investigating this possibility, we have synthesized a series of bivalent ligands 1-5 that contain both μ agonist and CB1 antagonist pharmacophores for use as tools to study the functional interaction between MOP and CB1 receptors in vivo. Immunofluorescent studies on HEK293 cells coexpressing both receptors suggested 5 (20-atom spacer) to be the only member of the series that bridges the protomers of the heteromer. Antinociceptive testing in mice revealed 5 to be the most potent member of the series. As neither a mixture of monovalent ligands 9 + 10 nor bivalents 2-5 produced tolerance in mice, MOR-CB1 apparently is not an important target for reducing tolerance.

Published

2013

14. Reduced Antinociception of Opioids in Rats and Mice by Vaccination with Immunogens Containing Oxycodone and Hydrocodone Haptens

Author

Paul R. Pentel, Morgan Le Naour, Marco Pravetoni, Theresa Harmon, Tara M. Hawley, Philip S. Portoghese, and A.M. Tucker

Subjects

Drug, Immunogen, media_common.quotation_subject, Enzyme-Linked Immunosorbent Assay, chemical and pharmacologic phenomena, Pharmacology, complex mixtures, Article, Mice, Pharmacotherapy, Drug Discovery, medicine, Animals, Hydrocodone, media_common, Vaccines, Synthetic, integumentary system, biology, Chemistry, hemic and immune systems, Rats, Analgesics, Opioid, Vaccination, biology.protein, Molecular Medicine, Haptens, Hapten, Oxycodone, Keyhole limpet hemocyanin, medicine.drug

Abstract

Prescription opioids abuse and associated deaths are an emerging concern in the USA. Vaccination against prescription opioids may provide an alternative to pharmacotherapy. An oxycodone hapten containing a tetraglycine linker at the C6 position (6OXY(Gly)(4)OH) conjugated to keyhole limpet hemocyanin (KLH) has shown early proof-of-efficacy in rodents as a candidate immunogen (6OXY(Gly)(4)-KLH) for the treatment of oxycodone abuse. In this study, oxycodone-based and hydrocodone-based haptens were conjugated to KLH to generate immunogens that would recognize both oxycodone and hydrocodone. Vaccination with 6OXY(Gly)(4)-KLH increased drug binding in serum, reduced drug distribution to brain, and blunted analgesia for both oxycodone and hydrocodone. An analogous C6-linked hydrocodone vaccine blocked hydrocodone effects but less so than 6OXY(Gly)(4)-KLH. C8-Linked hydrocodone immunogens had only limited efficacy. Amide conjugation showed higher haptenation ratios and greater efficacy than thioether conjugation to maleimide activated KLH (mKLH). The 6OXY(Gly)(4)-KLH vaccine may be used for treatment of prescription opioid abuse.

Published

2013

15. Modulation of Musculoskeletal Hyperalgesia by Brown Adipose Tissue Activity in Mice

Author

Myra G. Nunez, Philip S. Portoghese, Katalin J. Kovács, Elizabeth M Goudie-DeAngelis, Casey L. Kissel, Ramy E. Abdelhamid, and Alice A. Larson

Subjects

0301 basic medicine, Male, Pain Threshold, Tail, medicine.medical_specialty, Adrenergic receptor, Adipose tissue, Article, Body Temperature, 03 medical and health sciences, Mice, 0302 clinical medicine, Adipose Tissue, Brown, Musculoskeletal Pain, Internal medicine, Brown adipose tissue, Adrenergic antagonist, Reaction Time, Medicine, Animals, Chronic stress, Adrenergic agonist, Muscle Strength, Swimming, Uncoupling Protein 1, Mice, Knockout, business.industry, Body Weight, Adrenergic beta-Agonists, Cold Temperature, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Anesthesiology and Pain Medicine, Endocrinology, medicine.anatomical_structure, Neurology, Ethanolamines, Hyperalgesia, Female, Neurology (clinical), medicine.symptom, business, Thermogenesis, 030217 neurology & neurosurgery

Abstract

Cold exposure and a variety of types of mild stress increase pain in patients suffering from painful disorders such as fibromyalgia syndrome. Acutely, stress induces thermogenesis by increasing sympathetic activation of beta-3 (β3) adrenergic receptors in brown adipose tissue. Chronic stress leads to the hypertrophy of brown adipose, a phenomenon termed adaptive thermogenesis. Based on the innervation of skeletal muscle by collaterals of nerves projecting to brown adipose, we theorized an association between brown adipose tissue activity and musculoskeletal hyperalgesia and tested this hypothesis in mice. Exposure to a cold swim or injection of BRL37344 (β3 adrenergic agonist) each enhanced musculoskeletal hyperalgesia, as indicated by morphine-sensitive decreases in grip force responses, whereas SR59230A (β3 adrenergic antagonist) attenuated swim-induced hyperalgesia. Chemical ablation of interscapular brown adipose, using Rose Bengal, attenuated the development of hyperalgesia in response to either swim stress or BRL37344. In addition, elimination of the gene expressing uncoupling protein-1 (UCP1), the enzyme responsible for thermogenesis, prevented musculoskeletal hyperalgesia in response to either a swim or BRL37344, as documented in UCP1-knock out (UCP1-KO) mice compared to wild type controls. Together these data provide a convergence of evidence suggesting that activation of brown adipose contributes to stress-induced musculoskeletal hyperalgesia.

Published

2016

16. An Oxycodone Conjugate Vaccine Elicits Drug-Specific Antibodies that Reduce Oxycodone Distribution to Brain and Hot-Plate Analgesia

Author

M. Le Naour, Philip S. Portoghese, Marco Pravetoni, A.M. Tucker, Paul R. Pentel, and Theresa Harmon

Subjects

Male, Hot Temperature, Dose-Response Relationship, Immunologic, Pain, chemical and pharmacologic phenomena, Pharmacology, Antibodies, Rats, Sprague-Dawley, Drug Discovery and Translational Medicine, Therapeutic index, medicine, Animals, Bovine serum albumin, Pain Measurement, Vaccines, Conjugate, integumentary system, biology, Chemistry, Brain, Rats, Opioid, Oxymorphone, Antibody Formation, biology.protein, Morphine, Molecular Medicine, Cattle, Analgesia, Chickens, Oxycodone, Keyhole limpet hemocyanin, Protein Binding, medicine.drug, Buprenorphine

Abstract

Opioid conjugate vaccines have shown promise in attenuating the behavioral effects of heroin or morphine in animals. The goal of this study was to extend this approach to oxycodone (OXY), a commonly abused prescription opioid. Haptens were generated by adding tetraglycine (Gly)(4) or hemisuccinate (HS) linkers at the 6-position of OXY. Immunization of rats with OXY(Gly)(4) conjugated to the carrier proteins bovine serum albumin (BSA) or keyhole limpet hemocyanin (KLH) produced high-titer antibodies to OXY and its metabolite oxymorphone with substantially lower affinities for other structurally related opioid agonists and antagonists. There was no measurable binding of antibody by the (Gly)(4) linker alone or off-target opioids methadone and buprenorphine. OXY(HS) conjugates were less immunogenic despite achieving protein haptenation ratios comparable to OXY(Gly)(4)-BSA. In rats given a single intravenous dose of OXY, immunization with OXY(Gly)(4)-KLH increased OXY protein binding and retention in serum while decreasing its unbound (free) concentration in plasma and distribution to brain. Vaccine efficacy correlated with serum antibody titers, and it was greatest in rats given the lowest OXY dose (0.05 mg/kg) but was significant even after a larger OXY dose (0.5 mg/kg), equivalent to the high end of the therapeutic range in humans. These effects of OXY(Gly)(4)-KLH on drug disposition were comparable to those of nicotine or cocaine vaccines that are in clinical trials as addiction treatments. Immunization with OXY(Gly)(4)-KLH also reduced OXY analgesia in a thermal nociception test. These data support further study of vaccination with the OXY(Gly)(4)-KLH immunogen as a potential treatment option for OXY abuse or addiction.

Published

2012

17. A κ Opioid Pharmacophore Becomes a Spinally Selective κ-δ Agonist When Modified with a Basic Extender Arm

Author

Michael D. Powers, Jie Yang, Ye Tang, Philip S. Portoghese, and Mary M. Lunzer

Subjects

Agonist, medicine.drug_class, Chemistry, Organic Chemistry, Pharmacology, Biochemistry, Nociception, Opioid, In vivo, Opioid receptor, Drug Discovery, medicine, Potency, Pharmacophore, Receptor, medicine.drug

Abstract

We have explored the concept of a molecular extender arm attached to a κ opioid agonist pharmacophore 3 (ICI-199,441) in an effort to potentially interact with a complementary group on a neighboring opioid receptor. The molecular arm containing a terminal amine group was lengthened incrementally from 11 up to 18 atoms. Increasing the number of atoms in the arm produced virtually no change in the mouse intracerebroventricular (i.c.v.) antinociceptive potency. In contrast, the intrathecal (i.t.) potency of 6 (KDA-16) with a 16-atom arm was dramatically increased, as reflected by its antinociceptive i.c.v./i.t. ED50 ratio of ∼130. Further lengthening led to a decreased ED50 ratio. In vivo selective antagonist studies of KDA-16 revealed that κ and δ opioid receptors were responsible for the greatly enhanced i.t. potency. Calcium release experiments in HEK-293 cells suggested that KDA-16 selectively activate κ-δ heteromers. These data are consistent with the reported possible presence of heteromeric κ-δ opioid receptors in mouse spinal cord but not in the brain. The use of a molecular extender arm may be useful for developing spinally selective analgesics.

Published

2010

18. Modulation of Cell Surface Expression of Nonactivated Cholecystokinin Receptors Using Bivalent Ligand-Induced Internalization

Author

Philip S. Portoghese, Eyup Akgün, Kaleeckal G. Harikumar, and Laurence J. Miller

Subjects

Agonist, medicine.drug_class, Stereochemistry, media_common.quotation_subject, Receptors, Opioid, mu, Down-Regulation, CHO Cells, Immune receptor, Ligands, Cholecystokinin receptor, Article, Substrate Specificity, Cricetulus, Cricetinae, Chlorocebus aethiops, Drug Discovery, Enzyme-linked receptor, medicine, Animals, 5-HT5A receptor, Internalization, Receptor, media_common, Chemistry, Receptor antagonist, Endocytosis, Gene Expression Regulation, COS Cells, Biophysics, Molecular Medicine, Receptors, Cholecystokinin

Abstract

CCK(2) receptor antagonists potentiate pain relief by MOP receptor agonists. In an attempt to enhance this effect, we prepared bivalent ligands incorporating CCK(2) receptor antagonist and MOP receptor agonist pharmacophores. (9) Ligands with 16- to 22-atom spacers could simultaneously bind both receptors but provided no advantage in activity over individual ligands. We now examine the effect of these ligands on receptor internalization as a mechanism of receptor regulation. We prepared CHO cell lines expressing nonfluorescent halves (YN and YC) of yellow fluorescent protein attached to each receptor. Spatial approximation of constructs was needed to yield fluorescence. Monovalent MOP agonist 1 signaled normally and internalized the MOP receptor. Monovalent CCK(2) antagonist 2 did not stimulate receptor internalization. In the dual receptor-bearing cells, bivalent ligands 3a-c capable of simultaneously binding both receptors resulted in cell surface fluorescence and internalization of the fluorescent complex in a time- and temperature-dependent manner. Bivalent ligand 4 with spacer too short to occupy both receptors simultaneously yielded no signal. Receptor tethering with appropriate bivalent ligands can down-regulate signaling by moving a nonactivated receptor into the endocytic pathway.

Published

2010

19. Standard Opioid Agonists Activate Heteromeric Opioid Receptors: Evidence for Morphine and [<scp>d</scp>-Ala2-MePhe4-Glyol5]Enkephalin as Selective μ−δ Agonists

Author

Ajay S. Yekkirala, Alexander E. Kalyuzhny, and Philip S. Portoghese

Subjects

Agonist, medicine.medical_specialty, Pyrrolidines, Enkephalin, Physiology, medicine.drug_class, Cognitive Neuroscience, Benzeneacetamides, Receptors, Opioid, mu, Pharmacology, Ligands, Biochemistry, OGFr, chemistry.chemical_compound, Receptors, Opioid, delta, Internal medicine, medicine, Functional selectivity, Humans, Calcium Signaling, Receptor, Morphine, Receptors, Opioid, kappa, Cell Biology, General Medicine, Enkephalin, Ala(2)-MePhe(4)-Gly(5), Immunohistochemistry, Analgesics, Opioid, DAMGO, HEK293 Cells, Endocrinology, chemistry, Opioid, Guanosine 5'-O-(3-Thiotriphosphate), Area Under Curve, Receptors, Opioid, Bremazocine, Enkephalin, D-Penicillamine (2,5), medicine.drug

Abstract

Research in the opioid field has relied heavily on the use of standard agonist ligands such as morphine, [d-Ala(2)-MePhe(4)-Glyol(5)]enkephalin (DAMGO), U69593, bremazocine, [d-Pen(2)d-Pen(5)]enkephalin (DPDPE), and deltorphin-II as tools for investigating the three major types of opioid receptors, MOP (μ), KOP (κ), and DOP (δ), that mediate antinociception. The functional selectivity of these ligands has been based on the assumption that opioid receptors exist as homomers. As numerous studies in cultured cells have suggested that opioid receptors can associate both as homomers and heteromers, we have investigated the selectivity of these standard ligands using intracellular calcium release and [(35)S]GTPγS assays in HEK-293 cells that contain singly and coexpressed opioid receptors. The present study reveals that morphine and DAMGO, traditionally classified as μ selective agonists, selectively activate μ-δ heteromeric opioid receptors with greater efficacy than homomeric opioid receptors. Moreover, standard ligands that have been widely employed as κ- and δ-selective agonists display little or no differences in the activation of homomeric and heteromeric opioid receptors. The far-reaching implications of these results are discussed.

Published

2009

20. Morphine Tolerance in Mice Changes Response of Heroin from μ to δ Opioid Receptors

Author

Philip S. Portoghese, Blythe B. Holmes, James M. Fujimoto, and Jodie J. Rady

Subjects

Agonist, medicine.medical_specialty, medicine.drug_class, Chemistry, Pharmacology, Receptor antagonist, General Biochemistry, Genetics and Molecular Biology, Endocrinology, Opioid, Naltriben, Opioid receptor, Naltrindole, Internal medicine, Morphine, medicine, μ-opioid receptor, medicine.drug

Abstract

Heroin produced antinociception in the tail flick test through mu receptors in the brain of ICR and CD-1 mice, a response inhibited by 3-O-methylnaltrexone. Tolerance to morphine was produced by subcutaneous morphine pellet implantation. By the third day, the heroin response was produced through delta opioid receptors. The response was inhibited by simultaneous intracerebroventricular (i.c. v.) administration of naltrindole, a delta opioid receptor antagonist. More specifically, delta1 rather than delta2 receptors were involved because 7-benzylidenenaltrexone, a delta1 receptor antagonist, inhibited but naltriben, a delta2 antagonist, did not. Also, antinociception produced by i.c.v. heroin was inhibited by intrathecal administration of bicuculline and picrotoxin consistent with the concept that delta1 receptors in the brain mediated the antinociceptive response through descending neuronal pathways to the spinal cord to activate GABAA and GABAB receptors rather than spinal alpha2-adrenergic and serotonergic receptors activated originally by the mu agonist action in naive mice. The mu response of 6-monoacetylmorphine, a metabolite of heroin, was changed by morphine pellet implantation to a delta2 response (inhibited by naltriben but not 7-benzylidenenaltrexone). The agonist action of morphine in these morphine-tolerant mice remained mu. Thus, the opioid receptor selectivity of heroin and 6-monoacetylmorphine in the brain is changed by production of tolerance to morphine. Such a change explains how morphine tolerant mice are not cross-tolerant to heroin.

Published

2008

21. o-Naphthalenedicarboxaldehyde Derivative of 7‘-Aminonaltrindole as a Selective δ-Opioid Receptor Affinity Label

Author

Yan Zhang, Bertrand Le Bourdonnec, Sarika Prabhu Haris, Christopher R. McCurdy, and Philip S. Portoghese

Subjects

Conformational change, Magnetic Resonance Spectroscopy, Schiff base, biology, medicine.drug_class, Chemistry, Stereochemistry, Narcotic Antagonists, Affinity label, Antagonist, Affinity Labels, Carboxamide, Spectrometry, Mass, Fast Atom Bombardment, Naltrexone, chemistry.chemical_compound, Opioid receptor, Receptors, Opioid, delta, Drug Discovery, medicine, biology.protein, Molecular Medicine, Moiety, Derivative (chemistry)

Abstract

Incorporation of a naphthalene-dialdehyde moiety into the delta antagonist, 6'-aminonaltrindole afforded a potent, selective, irreversible delta-agonist 1. However, flow cytometry studies revealed no time-dependent specific fluorescence, suggesting that both Lys214 and Cys216 at the recognition site are not involved in covalent binding. Molecular simulation studies suggest that compound 1 may form a Schiff base with the epsilon-amino group of Lys214, which could explain its irreversibility and transformation into a delta-agonist through a conformational change of TM5.

Published

2007

22. Synthesis and124I-labeling ofm-iodophenylpyrrolomorphinan as a potential PET imaging agent for delta opioid (DOP) receptors

Author

Munawwar Sajjad, Eyup Akgün, Hani A. Nabi, and Philip S. Portoghese

Subjects

Agonist, medicine.drug_class, Stereochemistry, Organic Chemistry, chemistry.chemical_element, Biological activity, Zinc, Biochemistry, Chemical synthesis, Analytical Chemistry, chemistry.chemical_compound, Acetic acid, chemistry, Oxymorphone, Drug Discovery, medicine, Radiology, Nuclear Medicine and imaging, Receptor, Sodium acetate, Spectroscopy, Nuclear chemistry, medicine.drug

Abstract

Condensation of phenylazo-β-ketoamide 4 with oxymorphone 5 afforded an m-iodophenylpyrrolomorphinan (m-IPPM) 6 mediated by elemental zinc in acetic acid/sodium acetate buffer. m-IPPM 6 is a novel opioid receptor agonist (Ki = 4.53 nM for DOP) with high selectivity for DOP receptors. m-IPPM 6 was converted into the positron emitter m-[124I]PPM 8 via the stannylated intermediate 7. The final yield was 24.5 ± 1.9 % (n = 6) with a specific activity of 2.5 ± 1.2 Ci/µmol. Copyright © 2007 John Wiley & Sons, Ltd.

Published

2007

23. Inhibition of Inflammatory and Neuropathic Pain by Targeting a Mu Opioid Receptor/Chemokine Receptor5 Heteromer (MOR-CCR5)

Author

Eyup Akgün, Mary M. Lunzer, Yoshikazu Watanabe, Michael D. Powers, Yuk Y. Sham, Philip S. Portoghese, and Muhammad I. Javed

Subjects

Agonist, Male, Models, Molecular, Chemokine, Receptors, CCR5, medicine.drug_class, Heteromer, Receptors, Opioid, mu, CCR5 receptor antagonist, Pharmacology, Article, Chemokine receptor, Mice, Drug Discovery, medicine, Animals, Humans, Molecular Targeted Therapy, Inflammation, Analgesics, biology, Chemistry, HEK293 Cells, Opioid, CCR5 Receptor Antagonists, Chronic Disease, Morphine, biology.protein, Molecular Medicine, Neuralgia, μ-opioid receptor, medicine.drug

Abstract

Chemokine release promotes cross-talk between opioid and chemokine receptors that in part leads to reduced efficacy of morphine in the treatment of chronic pain. On the basis of the possibility that a MOR-CCR5 heteromer is involved in such cross-talk, we have synthesized bivalent ligands (MCC series) that contain mu opioid agonist and CCR5 antagonist pharmacophores linked through homologous spacers (14–24 atoms). When tested on lipopolysaccharide-inflamed mice, a member of the series (MCC22; 3e) with a 22-atom spacer exhibited profound antinociception (i.t. ED50 = 0.0146 pmol/mouse) that was 2000× greater than morphine. Moreover, MCC22 was ∼3500× more potent than a mixture of mu agonist and CCR5 antagonist monovalent ligands. These data strongly suggest that MCC22 acts by bridging the protomers of a MOR-CCR5 heteromer having a TM5,6 interface. Molecular simulation studies are consistent with such bridging. This study supports the MOR-CCR5 heteromer as a novel target for the treatment of chronic pain.

Published

2015

24. Opioid-induced tolerance and dependence in mice is modulated by the distance between pharmacophores in a bivalent ligand series

Author

Chris L. Etienne, Sandra C. Roerig, Philip S. Portoghese, Ping-Yee Law, David J. Daniels, and Natalie R. Lenard

Subjects

Male, Narcotics, Agonist, Time Factors, Stereochemistry, medicine.drug_class, Chemistry, Pharmaceutical, Narcotic Antagonists, Receptors, Opioid, mu, Physical dependence, Pharmacology, Ligands, Naltrexone, Mice, Naltrindole, Opioid receptor, Receptors, Opioid, delta, medicine, Animals, Analgesics, Mice, Inbred ICR, Models, Statistical, Multidisciplinary, Dose-Response Relationship, Drug, Morphine, Chemistry, Biological Sciences, Analgesics, Opioid, Models, Chemical, Opioid, Oxymorphone, medicine.symptom, medicine.drug

Abstract

Given the mounting evidence for involvement of δ opioid receptors in the tolerance and physical dependence of μ opioid receptor agonists, we have investigated the possible physical interaction between μ and δ opioid receptors by using bivalent ligands. Based on reports of suppression of antinociceptive tolerance by the δ antagonist naltrindole (NTI), bivalent ligands [μ-δ agonist-antagonist (MDAN) series] that contain different length spacers, and pharmacophores derived from NTI and the μ agonist oxymorphone, have been synthesized and evaluated by intracerebroventricular (i.c.v.) administration in the tail-flick test in mice. In acute i.c.v. studies, the bivalent ligands functioned as agonists with potencies ranging from 1.6- to 45-fold greater than morphine. In contrast, the monovalent μ agonist analogues were substantially more potent than the MDAN congeners and were essentially equipotent with one another and oxymorphone. Pretreatment with NTI decreased the ED 50 values for MDAN-19 to a greater degree than for MDAN-16 but had no effect on MDAN-21. Chronic i.c.v. studies revealed that MDAN ligands whose spacer was 16 atoms or longer produced less dependence than either morphine or μ monovalent control MA-19. On the other hand, both physical dependence and tolerance were suppressed at MDAN spacer lengths of 19 atoms or greater. These data suggest that physical interaction between the μ and δ opioid receptors modulates μ-mediated tolerance and dependence. Because MDAN-21 was found to be 50-fold more potent than morphine by the i.v. route (i.v.), it offers a previously uncharacterized approach for the development of analgesics devoid of tolerance and dependence.

Published

2005

25. Criteria for the safety evaluation of flavoring substances

Author

Samuel M. Cohen, Victor J. Feron, T. B. Adams, Robert L. Smith, Bernard M. Wagner, Jay I. Goodman, Philip S. Portoghese, William J. Waddell, I. C. Munro, John Doull, and Lawrence J. Marnett

Subjects

food.ingredient, business.industry, Food additive, food and beverages, Flavoring Agents, Context (language use), General Medicine, Toxicology, Biotechnology, Human health, food, Chemical groups, Medicine, Degree of confidence, business, S typhimurium, Flavor, Food Science

Abstract

The current status of the GRAS evaluation program of flavoring substances operated by the Expert Panel of FEMA is discussed. The Panel maintains a rigorous rotating 10-year program of continuous review of scientific data related to the safety evaluation of flavoring substances. The Panel concluded a comprehensive review of the GRAS (GRASa) status of flavors in 1985 and began a second comprehensive review of the same substances and any recently GRAS materials in 1994. This second re-evaluation program of chemical groups of flavor ingredients, recognized as the GRAS reaffirmation (GRASr) program, is scheduled to be completed in 2005. The evaluation criteria used by the Panel during the GRASr program reflects the significant impact of advances in biochemistry, molecular biology and toxicology that have allowed for a more complete understanding of the molecular events associated with toxicity. The interpretation of novel data on the relationship of dose to metabolic fate, formation of protein and DNA adducts, enzyme induction, and the cascade of cellular events leading to toxicity provides a more comprehensive basis upon which to evaluate the safety of the intake of flavor ingredients under conditions of intended use. The interpretation of genotoxicity data is evaluated in the context of other data such as in vivo animal metabolism and lifetime animal feeding studies that are more closely related to actual human experience. Data are not viewed in isolation, but comprise one component that is factored into the Panel's overall safety assessment. The convergence of different methodologies that assess intake of flavoring substances provides a greater degree of confidence in the estimated intake of flavor ingredients. When these intakes are compared to dose levels that in some cases result in related chemical and biological effects and the subsequent toxicity, it is clear that exposure to these substances through flavor use presents no significant human health risk.

Published

2005

26. The FEMA GRAS assessment of phenethyl alcohol, aldehyde, acid, and related acetals and esters used as flavor ingredients

Author

Bernard M. Wagner, Robert L. Smith, John Doull, Philip S. Portoghese, Lawrence J. Marnett, Samuel M. Cohen, William J. Waddell, I. C. Munro, Victor J. Feron, Jay I. Goodman, and T. B. Adams

Subjects

Phenylacetates, medicine.medical_treatment, Flavoring Agents, Context (language use), Acetaldehyde, Toxicology, chemistry.chemical_compound, Acetals, Detoxification (alternative medicine), Toxicity Tests, medicine, Animals, Food Industry, Humans, Organic chemistry, Flavor, United States Food and Drug Administration, food and beverages, Esters, General Medicine, Phenylethyl Alcohol, equipment and supplies, United States, Food Analysis, chemistry, Phenethyl alcohol, Food Science

Abstract

This publication is the ninth in a series of safety evaluations performed by the Expert Panel of the Flavor and Extract Manufacturers Association (FEMA). In 1993, the Panel initiated a comprehensive program to re-evaluate the safety of more than 1700 GRAS flavoring substances under conditions of intended use. Elements that are fundamental to the safety evaluation of flavor ingredients include exposure, structural analogy, metabolism, pharmacokinetics and toxicology. Flavor ingredients are evaluated individually and in the context of the available scientific information on the group of structurally related substances. Scientific data relevant to the safety evaluation of the use of phenethyl alcohol, aldehyde, acid, and related acetals and esters as flavoring ingredients is evaluated. The group of phenethylalcohol, aldehyde, acid, and related acetals and esters was reaffirmed as GRAS (GRASr) based, in part, on their self-limiting properties as flavoring substances in food, their rapid absorption, metabolic detoxication, and excretion in humans and other animals, their low level of flavor use, the wide margins of safety between the conservative estimates of intake and the no-observed-adverse effect levels determined from subchronic and chronic studies and the lack of significant genotoxic and mutagenic potential. This evidence of safety is supported by the fact that the intake of phenethyl alcohol, aldehyde, acid, and related acetals and esters as natural components of traditional foods is greater than their intake as intentionally added flavoring substances.

Published

2005

27. Interaction of Bivalent Ligand KDN21 with Heterodimeric δ-κ Opioid Receptors in Human Embryonic Kidney 293 Cells

Author

David J. Daniels, Philip S. Portoghese, Rashmi G. Bhushan, and Zhihua Xie

Subjects

Pharmacology, Chemistry, medicine.drug_class, Stereochemistry, Receptors, Opioid, kappa, Molecular Sequence Data, Kidney metabolism, Kidney, Ligands, κ-opioid receptor, Naltrexone, Cell Line, Naltriben, Naltrindole, Receptors, Opioid, delta, medicine, Molecular Medicine, Amino Acid Sequence, Phosphorylation, Diprenorphine, Norbinaltorphimine, Receptor, Oligopeptides, Opioid antagonist, medicine.drug

Abstract

KDN21 is a bivalent ligand that contains delta and kappa opioid antagonist pharmacophores linked through a 21-atom spacer. It has been reported that KDN21 bridges delta and kappa receptors that are organized as heterodimers. We have shown previously that when using [(3)H]diprenorphine as radioligand, KDN21 displayed greatly enhanced affinity in this series for coexpressed delta and kappa opioid receptors (CDK). The present study used in vitro expression systems to investigate interactions of members of the KDN series with delta-kappa heterodimers through competition binding using selective ligands and the mitogen-activated protein kinase (MAPK) assay. In this regard, the use of the selective radioligands [(3)H]naltrindole and [(3)H]norbinaltorphimine (nor-BNI) in competition binding studies revealed that KDN21 has much higher affinity than other KDN members for CDK and bound to CDK more selectively relative to mixed delta and kappa opioid receptors or singly expressed delta and kappa opioid receptors. Other experiments revealed that the binding of naltrindole to delta opioid receptors could increase the binding of nor-BNI to kappa opioid receptors and vice versa, suggesting reciprocal allosteric modulation of receptors in the heterodimer. Regarding the selectivity of KDN21 for phenotypic delta and kappa opioid receptors, we investigated the effect of KDN21 on the activation of MAPKs [extracellular signal-regulated kinases 1 and 2 (ERK1/2)] by delta- or kappa-selective agonists. KDN21 inhibited the activation of ERK1/2 by [D-Pen(2),D-Pen(5)]-enkephalin (delta(1)) and bremazocine (kappa(2)) but had no effect on the activation by deltorphin II (delta(2)) and (+)-(5alpha,7alpha,8beta)-N-methyl-N-[7-(1-pyrrolidinyl)-1-oxaspiro[4.5]dec-8-yl]benzeneacetamide (U69593, kappa(1)). 7-Benzylidenenaltrexone (delta(1)) and bremazocine (kappa(2)) significantly reduced the binding of KDN21 to CDK, whereas naltriben (delta(2)) and U69593 produced no such change. Taken together, these data support the idea that the organization of delta and kappa receptors as heterodimers gives rise to delta(1) and kappa(2) phenotypes.

Published

2005

28. Homology Modeling and Molecular Dynamics Simulations of the Mu Opioid Receptor in a Membrane-Aqueous System

Author

Yan Zhang, Philip S. Portoghese, Ramkumar Rajamani, Jiali Gao, and Yuk Y. Sham

Subjects

Models, Molecular, Rhodopsin, Molecular model, Stereochemistry, Receptors, Opioid, mu, Sequence Homology, Crystallography, X-Ray, Biochemistry, Naltrexone, Protein structure, medicine, Animals, Computer Simulation, Homology modeling, Lipid bilayer, Molecular Biology, G protein-coupled receptor, Binding Sites, biology, Chemistry, Cell Membrane, Organic Chemistry, Water, Lipid Metabolism, Lipids, Protein Structure, Tertiary, Structural Homology, Protein, Solvents, biology.protein, Molecular Medicine, Cattle, μ-opioid receptor, medicine.drug

Abstract

Three types of opioid receptors-mu, delta, and kappa-belong to the rhodopsin subfamily in the G protein-coupled receptor superfamily. With the recent characterization of the high-resolution X-ray crystal structure of bovine rhodopsin, considerable attention has been focused on molecular modeling of these transmembrane proteins. In this study, a homology model of the mu opioid receptor was constructed based on the X-ray crystal structure of bovine rhodopsin. A phospholipid bilayer was built around the receptor, and two water layers were placed on both surfaces of the lipid bilayer. Molecular-dynamics simulations were carried out by using CHARMM for the entire system, which consisted of 316 amino acid residues, 92 phospholipid molecules, 8327 water molecules, and 11 chloride counter ions-40 931 atoms altogether. The whole system was equilibrated for 250 ps followed by another 2 ns dynamic simulation. The opioid ligand naltrexone was docked into the optimized model, and the critical amino acid residues for binding were identified. The mu opioid receptor homology model optimized in a complete membrane-aqueous system should provide a good starting point for further characterization of the binding modes for opioid ligands. Furthermore, the method developed herein will be applicable to molecular model building to other opioid receptors as well as other GPCRs.

Published

2005

29. A Bivalent Ligand (KDAN-18) Containing δ-Antagonist and κ-Agonist Pharmacophores Bridges δ2 and κ1 Opioid Receptor Phenotypes

Author

Zhihua Xie, David J. Daniels, Rashmi G. Bhushan, Philip S. Portoghese, and Amol Kulkarni

Subjects

Agonist, medicine.drug_class, Chemistry, Stereochemistry, Antagonist, Opioid, Opioid receptor, Naltrindole, Drug Discovery, medicine, Molecular Medicine, Pharmacophore, Receptor, Kappa, medicine.drug

Abstract

To characterize delta- and kappa-opioid receptor phenotypes, bivalent ligands (KDAN series) containing delta-antagonist (naltrindole) and kappa(1)-agonist (ICI-199,441) pharmacophores were synthesized and evaluated by the intrathecal route using the mouse tail-flick assay and binding studies. The data have suggested that KDAN-18 (2) bridges phenotypic delta(2)- and kappa(1)-receptors. A conceptual model is presented to explain the organizational differences between the opioid receptors that give rise to the phenotypes (delta(1), delta(2), kappa(1), kappa(2)).

Published

2004

30. A Bivalent Ligand (KDN-21) Reveals Spinal δ and κ Opioid Receptors Are Organized as Heterodimers That Give Rise to δ1 and κ2 Phenotypes. Selective Targeting of δ−κ Heterodimers

Author

Shiv Kumar Sharma, David J. Daniels, Rashmi G. Bhushan, Zhihua Xie, and Philip S. Portoghese

Subjects

medicine.drug_class, Chemistry, Ligand, Stereochemistry, Central nervous system, Bivalent (genetics), medicine.anatomical_structure, Opioid, Opioid receptor, Drug Discovery, medicine, Molecular Medicine, Structure–activity relationship, Pharmacophore, Receptor, medicine.drug

Abstract

In view of recent pharmacological studies suggesting the existence of δ−κ opioid receptor heterodimers/oligomers in the spinal cord, we have synthesized and evaluated (intrathecally in mice) a series of bivalent ligands (KDN series) containing κ and δ antagonist pharmacophores. Pharmacological and binding data have provided evidence for the bridging of spinal δ−κ receptor heterodimers by KDN-21 and for their identification as δ1 and κ2. The selectivity profile of KDN-21 and the apparent absence of coupled δ1−κ2 phenotypes in the brain suggest a new approach for targeting receptors.

Published

2004

31. Characterization of Specific Opioid Binding Sites in Neural Membranes from the Myenteric Plexus of Porcine Small Intestine

Author

David R. Brown, Philip S. Portoghese, and DeWayne Townsend

Subjects

Male, Narcotics, Agonist, medicine.medical_specialty, Enkephalin, Swine, Stereochemistry, medicine.drug_class, Narcotic Antagonists, Receptors, Opioid, mu, Diprenorphine, Myenteric Plexus, (+)-Naloxone, Tritium, Receptors, Opioid, delta, Internal medicine, Intestine, Small, medicine, Animals, Drug Interactions, Binding site, Receptor, Myenteric plexus, Pharmacology, Binding Sites, Chemistry, Receptors, Opioid, kappa, Cell Membrane, Sodium, Endocrinology, Naltriben, Molecular Medicine, Female, Enkephalin, D-Penicillamine (2,5), HEPES, medicine.drug

Abstract

Delta- and kappa-opioid receptors (OPRs), but not micro-OPRs, are expressed in the myenteric plexus of the porcine distal small intestine. In a subpopulation of myenteric neurons, delta- and kappa-OPRs seem to be colocalized and may functionally interact. In this study, radioligand binding was used to characterize myenteric OPR populations in detail. The nonselective OPR antagonist [3H]diprenorphine bound to a single, high-affinity site in myenteric neural membrane homogenates. Naloxone displaced 65 and 59% of [3H]diprenorphine binding from this site in Na(+)-free Tris and Krebs-HEPES buffers, respectively. Naltrexone-derived delta- and kappa-OPR antagonists, including naltriben, 7-benzylidenenaltrexone, nor-binaltorphimine, and 5'-guanidinonaltrindole, displaced [3H]diprenorphine from two distinct binding sites to levels similar to that of naloxone. The selective delta-OPR ligands Tyr-1,2,3,4-tetrahydroisoquinoline-Phe-Phe-OH (TIPP), [D-Pen2,D-Pen5]enkephalin (DPDPE), [D-Ala2, Glu4]deltorphin II, and (+)-4-[(alphaR)-alpha((2S,5R)-4-allyl-2,5-dimethyl-1-piperazinyl-3-methoxybenzyl)-N,N-diethylbenzamide (SNC-80) and the kappa-OPR agonist (D-(5alpha,7alpha,8beta)-(-)-N-methyl-N-(7-(1-pyrrolidinyl)-1-oxoaspiro-(4,5)dec-8-yl) benzeneacetamide (U-69,593) displaced [3H]diprenorphine from three independent binding sites; these included high-affinity delta- and kappa-OPR sites, and a residual binding site. Residual [3H]diprenorphine binding was displaced by the selective kappa-OPR antagonist nor-binaltorphimine after saturation of delta and kappa sites, respectively, with DPDPE and U-69,593. The residual binding site displayed low affinity for delta- and kappa-OPR agonists and TIPP, as well as moderate affinity for naltrexone-derived ligands, properties reminiscent of delta-/kappa-OPR heterodimers.

Published

2003

32. Antidepressant-Like Effects of κ-Opioid Receptor Antagonists in the Forced Swim Test in Rats

Author

William A. Carlezon, William C. Stevens, Mark S. Todtenkopf, Philip S. Portoghese, Hilarie C. Tomasiewicz, Stephen D. Mague, Andrea M. Pliakas, Robert M. Jones, and Yan Zhang

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Narcotic Antagonists, Dynorphin, Motor Activity, Nucleus accumbens, Citalopram, Pharmacology, CREB, Rats, Sprague-Dawley, Opioid receptor, Internal medicine, Desipramine, medicine, Animals, Swimming, biology, Receptors, Opioid, kappa, Antidepressive Agents, Rats, Endocrinology, Brain stimulation, Models, Animal, biology.protein, Molecular Medicine, Psychology, Behavioural despair test, medicine.drug

Abstract

We showed previously that cAMP response element-binding protein (CREB) within the nucleus accumbens (NAc) of rats regulates immobility in the forced swim test (FST), an assay used to study depression. Because CREB regulates expression of dynorphin (which acts at kappa-opioid receptors) in NAc neurons, these findings raised the possibility that kappa-receptors mediate immobility behaviors in the FST. Here, we report that i.c.v. administration of the kappa-antagonist nor-binaltorphimine dose dependently decreased immobility in the FST, suggesting that it has antidepressant-like effects. Implicating a specific effect at kappa-receptors, similar antidepressant-like effects were seen after treatment with either of two novel, structurally dissimilar kappa-antagonists: 5'-guanidinonaltrindole, which was effective after i.c.v. but not systemic treatment, and 5'-acetamidinoethylnaltrindole (ANTI), which was potent and effective after systemic treatment. The behavioral effects of the kappa-antagonists resembled those of tricyclic antidepressants (desipramine) and selective serotonin reuptake inhibitors (fluoxetine and citalopram). Conversely, systemic administration of the kappa-agonist [5alpha,7alpha,8beta]-N-methyl-N-[7-[1-pyrrolidinyl]-1-oxaspiro[4.5]dec8-yl]-benzenacetamide (U-69593) dose dependently increased immobility in the FST, consistent with prodepressant-like effects. The effects of the kappa-ligands in the FST were not correlated with nonspecific effects on locomotor activity. Furthermore, the most potent and effective kappa-antagonist (ANTI) did not affect the rewarding impact of lateral hypothalamic brain stimulation at a dose with strong antidepressant-like effects. These findings are consistent with the hypothesis that CREB-mediated induction of dynorphin in the NAc "triggers" immobility behavior in the FST. Furthermore, they raise the possibility that kappa-antagonists may have efficacy as antidepressants, but lack stimulant or reward-related effects.

Published

2003

33. Kappa opioid antagonist effects of the novel kappa antagonist 5?-guanidinonaltrindole (GNTI) in an assay of schedule-controlled behavior in rhesus monkeys

Author

Robert M. Jones, Philip S. Portoghese, David C. Linsenmayer, S. Stevens Negus, and Nancy K. Mello

Subjects

Male, Narcotics, Agonist, medicine.medical_specialty, Pyrrolidines, Reinforcement Schedule, Time Factors, medicine.drug_class, Narcotic Antagonists, Benzeneacetamides, Pharmacology, Guanidines, κ-opioid receptor, Piperazines, chemistry.chemical_compound, Receptors, Opioid, delta, Internal medicine, 5'-Guanidinonaltrindole, medicine, Animals, Drug Interactions, Analgesics, Dose-Response Relationship, Drug, Morphine, business.industry, Receptors, Opioid, kappa, 3,4-Dichloro-N-methyl-N-(2-(1-pyrrolidinyl)-cyclohexyl)-benzeneacetamide, (trans)-Isomer, Antagonist, Analgesics, Non-Narcotic, JDTic, Macaca mulatta, Naltrexone, Endocrinology, Morphinans, Opioid, chemistry, Benzamides, Conditioning, Operant, Female, business, Opioid antagonist, medicine.drug

Abstract

Rationale: Opioid receptors are divided into three types: kappa, mu, and delta receptors. Receptor-selective antagonists are useful experimental tools for evaluation of opioid receptor-mediated processes. 5′-Guanidinonaltrindole (GNTI) was recently developed as a novel kappa-selective antagonist. Objectives: To evaluate the potency, time course, and selectivity of GNTI's opioid antagonist effects in rhesus monkeys in an assay of schedule-controlled responding. Methods: Five rhesus monkeys were trained to respond under a fixed ratio 30 schedule of food reinforcement. The rate-decreasing effects of the kappa agonists U50,488 and U69,593, the mu agonist morphine, and the delta agonist SNC80 were examined alone and after pretreatment with GNTI (0.1 and 1.0 mg/kg i.m.; 1 h to 14 days). Results: U50,488, U69,593, morphine, and SNC80 dose-dependently decreased response rates in this procedure. GNTI produced a dose- and time-dependent antagonism of the rate-decreasing effects of U50,488. The kappa antagonist effects of GNTI had a slow onset and a long duration of action, and peak antagonist effects were observed after 24 h. A higher dose of 3.2 mg/kg GNTI eliminated responding in one monkey and was not studied further. The antagonist effects of GNTI were kappa selective, because 1.0 mg/kg GNTI also antagonized the effects of U69,593, but not those of morphine or SNC80. Conclusions: These results suggest that GNTI is a potent and selective kappa antagonist with a slow onset and long duration of action in rhesus monkeys. Relative to the prototype kappa antagonist nor-binaltorphimine, GNTI may have some advantages as a tool for the study of kappa receptor-mediated processes.

Published

2002

34. Methadone and Heroin Antinociception: Predominant £-Opioid-Receptor Responses in Methadone-Tolerant Mice

Author

James M. Fujimoto, Philip S. Portoghese, and Jodie J. Rady

Subjects

Agonist, Methadone maintenance, medicine.drug_class, Receptors, Opioid, mu, Pharmacology, Receptors, N-Methyl-D-Aspartate, Mice, Species Specificity, Opioid receptor, Receptors, Opioid, delta, medicine, Animals, 5-HT receptor, Injections, Intraventricular, Drug Implants, Dose-Response Relationship, Drug, Chemistry, Drug Tolerance, Bicuculline, Analgesics, Opioid, Heroin, Naltriben, Morphine, Methadone, medicine.drug

Abstract

Antinociceptive tail flick responses to heroin and 6-monoacetylmorphine mediated in the brain by mu-opioid receptor are switched by morphine pellet implantation to delta1- and delta2-opioid-receptors mediation, respectively. Present results showed that the mu-receptor response (inhibited by beta-funaltrexamine) to methadone was changed by morphine pellet implantation to delta1 (inhibited by 7-benzylidenenaltrexone)- and delta2 (inhibited by naltriben)-opioid-receptor responses. Methadone pellet implantation likewise changed mediation from mu- to delta-opioid receptors for heroin and methadone but not for morphine (beta-funaltrexamine continued to inhibit). Methadone mu action in the brain was linked through a descending system to activate spinal serotonin receptors (inhibited by methysergide), but this link was gone in the methadone-pellet-implanted group. In the latter group, the new delta1- and delta2-receptor responses were mediated by spinal GABAA (inhibited by bicuculline) and GABAB (inhibited by 2-hydroxysaclofen) receptors. These shifts in neuronal systems meant that mu receptors on a given neuron were not changed into delta receptors. Preliminary results showed that delta-agonist action for methadone was prevented from appearing by MK801, a NMDA-receptor antagonist, and did not occur in 129S6/SvEv mice which lack NMDA responsiveness. Could methadone maintenance treatment in humans uncover delta-agonist actions?

Published

2002

35. Transformation of a κ-Opioid Receptor Antagonist to a κ-Agonist by Transfer of a Guanidinium Group from the 5‘- to 6‘-Position of Naltrindole

Author

David M. Ferguson, Shiv Kumar Sharma, Philip S. Portoghese, Robert M. Jones, and Thomas G. Metzger

Subjects

Conformational change, Stereochemistry, medicine.drug_class, Narcotic Antagonists, Guinea Pigs, Molecular Conformation, In Vitro Techniques, Transfection, Cell Line, Structure-Activity Relationship, Opioid receptor, Naltrindole, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Cloning, Molecular, Receptor, Guanidine, Chemistry, Receptors, Opioid, kappa, Antagonist, Muscle, Smooth, Biological activity, Naltrexone, Rats, Transmembrane domain, Mutagenesis, Site-Directed, Molecular Medicine, Muscle Contraction, medicine.drug

Abstract

The importance of the indole scaffold of GNTI 3 in directing its address (5'-guanidinium group) to associate with the Glu297 residue of the kappa-opioid receptor was investigated by the synthesis and biological evaluation of its 4'- (4a), 6'- (4b), and 7'- (4c) regioisomers. The finding that only the 5'-regioisomer (GNTI) possessed potent kappa-opioid antagonist activity and high affinity at kappa-receptors illustrates the importance of the 5'-position in orienting the guanidinium group to the proper recognition locus (Glu 297) for potent kappa-antagonist activity. The discovery that the 6'-regioisomer of GNTI was a potent kappa-agonist, together with the results of site-directed mutagenesis studies that are consistent with association between the 6'-guanidinium group and Glu297, suggest that the transition from an inactive to an active state of the kappa-receptor involves a conformational change of TM6. We propose that association of the 6'-guanidinium group of 4b with Glu297 promotes axial rotational motion of transmembrane helix VI which leads to receptor activation via a conformational change of inner loop 3.

Published

2001

36. From Models to Molecules: Opioid Receptor Dimers, Bivalent Ligands, and Selective Opioid Receptor Probes

Author

Philip S. Portoghese

Subjects

Molecular model, Chemistry, medicine.drug_class, Stereochemistry, Morphine derivatives, Bivalent (genetics), Opioid receptor, Drug Discovery, medicine, Molecular Medicine, Molecule, Norbinaltorphimine, Morphinan derivatives, medicine.drug

Published

2001

37. κ-Opioid receptor agonist suppression of HIV-1 expression in CD4+ lymphocytes

Author

An Chih Chang, Phillip K. Peterson, Genya Gekker, Xingin Fang, Jean M. Bidlack, Philip S. Portoghese, and James R. Lokensgard

Subjects

CD4-Positive T-Lymphocytes, Agonist, medicine.medical_specialty, medicine.drug_class, Lymphocyte, Cell, U-50488, In Vitro Techniques, Pharmacology, Biology, Biochemistry, Internal medicine, Gene expression, medicine, Humans, Receptor, Receptors, Opioid, kappa, 3,4-Dichloro-N-methyl-N-(2-(1-pyrrolidinyl)-cyclohexyl)-benzeneacetamide, (trans)-Isomer, Biological activity, Analgesics, Non-Narcotic, Flow Cytometry, In vitro, medicine.anatomical_structure, Endocrinology, HIV-1

Abstract

Synthetic κ-opioid receptor (KOR) agonists have been shown to suppress HIV-1 expression in acutely infected macrophages. In the present study, we examined the effects of the KOR ligand trans -3,4-dichloro- N -methyl- N [2-(1-pyrolidinyl)cyclohexyl]benzeneaceamide methanesulfonate (U50,488) on HIV-1 expression in CD4 + lymphocytes, the main target cell of this virus. When U50,488 was added to activated CD4 + lymphocytes, HIV-1 expression was inhibited in a concentration- and time-dependent manner with maximal suppression (≈60%) at 10 -7 M U50,488. The KOR selective antagonist nor-binaltorphimine (nor-BNI) had no effect by itself on viral expression but blocked the antiviral property of U50,488, suggesting that U50,488 was acting via a KOR-related mechanism. Support for the involvement of KOR was provided by the findings that 34% of activated CD4 + lymphocytes were positive for KOR, using an immunofluorescence technique, and that seven additional synthetic KOR ligands also inhibited HIV-1 expression. The results of this study broaden understanding of the antiviral properties of KOR ligands to include cells outside of the nervous system and suggest a potential role for these agents in the treatment of HIV-1 infection.

Published

2001

38. Affinity labels as tools for the identification of opioid receptor recognition sites

Author

Rachid El Kouhen, Philip S. Portoghese, Ping Y. Law, Bertrand Le Bourdonnec, and Horace H. Loh

Subjects

Binding Sites, biology, Chemistry, Stereochemistry, medicine.drug_class, Affinity label, Pharmaceutical Science, Affinity Labels, Biochemistry, Opioid receptor, Receptors, Opioid, Drug Discovery, medicine, biology.protein, Humans, μ-opioid receptor, Binding site, Pharmacophore, Receptor, Opioid antagonist, Endogenous agonist

Abstract

Affinity labels have proven to be useful tools in opioid research. We review experiments carried out with the mu opioid receptor affinity label, beta-funaltrexamine (2), that support the concept of different recognition sites for mu opioid agonists and antagonists. The data are interpreted in the context of a dimeric receptor that contains two allosterically coupled binding sites: one that binds endogenous agonist, and the second that functions as an inhibitory modulator of agonism. It is proposed that exogenous antagonists bind selectively to the second site. The first of a new class of affinity labels, PGNA (5), that contains the phthaldehyde moiety attached to an opioid antagonist pharmacophore, is described. This class of ligands has been named 'reporter affinity labels' because covalent association leads to the formation of a fluorescent isoindole that is diagnostic for cross-linking of lysine and cysteine residues. PGNA binds opioid receptors covalently, as suggested by (a) irreversible binding to cloned opioid receptors, (b) irreversible opioid antagonism in the guinea pig ileum preparation, and (c) ultra-long opioid antagonism in mice. Since flow cytometry experiments revealed specific enhancement of fluorescence in cloned mu receptors after a 1 min exposure to 5, it is concluded that covalent binding has occurred via the formation of an isoindole, presumably by cross-linking neighboring lysine and cysteine residues in the vicinity of the receptor recognition site.

Published

2001

39. Covalently Induced Activation of the δ Opioid Receptor by a Fluorogenic Affinity Label, 7‘-(Phthalaldehydecarboxamido)naltrindole (PNTI)

Author

Gennady Poda, Horace H. Loh, Philip S. Portoghese, Ping Y. Law, David M. Ferguson, Rachid El Kouhen, and Bertrand Le Bourdonnec

Subjects

Male, Models, Molecular, Agonist, Stereochemistry, medicine.drug_class, Affinity label, Guinea Pigs, CHO Cells, In Vitro Techniques, Ligands, Chemical synthesis, δ-opioid receptor, Mice, Vas Deferens, Ileum, Naltrindole, Cricetinae, Receptors, Opioid, delta, Drug Discovery, medicine, Animals, Fluorescent Dyes, Analgesics, biology, Chemistry, Affinity Labels, Biological activity, Naltrexone, In vitro, Covalent bond, biology.protein, Molecular Medicine, medicine.drug

Published

2001

40. Potent and Selective Indolomorphinan Antagonists of the Kappa-Opioid Receptor

Author

William C. Stevens, Thomas G. Metzger, Robert M. Jones, Philip S. Portoghese, David M. Ferguson, and Govindan Subramanian

Subjects

Models, Molecular, Indoles, Stereochemistry, Narcotic Antagonists, Transfection, Guanidines, κ-opioid receptor, Cell Line, Structure-Activity Relationship, chemistry.chemical_compound, Naltrindole, Drug Discovery, medicine, Humans, Moiety, Indole test, Morphine Derivatives, Receptors, Opioid, kappa, Antagonist, JDTic, Naltrexone, Morphinans, chemistry, Molecular Medicine, Norbinaltorphimine, Kappa, medicine.drug

Abstract

The indole moiety in the delta-opioid antagonist, naltrindole (2, NTI), was employed as a scaffold to hold an "address" for interaction with the kappa-opioid receptor. The attachment of the address to the 5'-position of the indole moiety was based on superposition of NTI upon the kappa antagonist, norbinaltorphimine (1, norBNI). A variety of cationic groups were employed as a kappa address in an effort to investigate its interaction with the anionic address subsite, Glu297, on the kappa receptor. Some of the groups that were employed for this purpose were amines, amidines, guanidines, and quaternary ammonium. Members of the series were found to have a varying degree of kappa antagonist potency and kappa selectivity when tested in smooth muscle preparations. The 5'-guanidine derivative 12a (GNTI) was the most potent member of the series and had the highest kappa selectivity ratio. GNTI was 2 times more potent and 6-10-fold more selective than norBNI (1). In general, the order of potency in the series was: guanidinesamidines approximately quaternary ammoniumamines. The kappa antagonist potency appeared to be a function of a combination of the pK(a) and distance constraint of the cationic substituent of the ligand. Receptor binding studies were qualitatively in agreement with the pharmacological data. Molecular modeling studies on 12a suggested that the protonated N-17 and guanidinium groups of GNTI are associated with Asp138 (TM3) and Glu297 (TM6), respectively, while the phenolic hydroxyl may be involved in donor-acceptor interactions with the imidazole ring of His291. It was concluded that the basis for the high kappa selectivity of GNTI is related both to association with the nonconserved Glu297 residue and to unfavorable interactions with an equivalent position in mu- and delta-opioid receptors.

Published

2000

41. 5′-Guanidinonaltrindole, a highly selective and potent κ-opioid receptor antagonist

Author

Robert M. Jones and Philip S. Portoghese

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Guinea Pigs, CHO Cells, In Vitro Techniques, Pharmacology, Ligands, Guanidines, Mice, chemistry.chemical_compound, Opioid receptor, Cricetinae, Internal medicine, 5'-Guanidinonaltrindole, medicine, Animals, Humans, Mice, Inbred ICR, Membranes, Chemistry, Receptors, Opioid, kappa, Antagonist, Muscle, Smooth, Enkephalin, Ala(2)-MePhe(4)-Gly(5), JDTic, Receptor antagonist, Naltrexone, Endocrinology, Morphinans, Competitive antagonist, Enkephalin, D-Penicillamine (2,5), Norbinaltorphimine, Opioid antagonist, medicine.drug

Abstract

5′-Guanidinonaltrindole (GNTI) possesses 5-fold greater opioid antagonist potency ( K e =0.04 nM) and an order of magnitude greater selectivity (selectivity ratios >500) than the prototypical κ-opioid receptor antagonist, norbinaltorphimine, in smooth muscle preparations. Binding and functional studies conducted on cloned human opioid receptors expressed in Chinese hamster ovarian (CHO) cells afforded pA 2 values that were comparable to the smooth muscle data. In view of the high selectivity and potency of GNTI, it is a potentially valuable pharmacological tool for opioid research.

Published

2000

42. Molecular Docking Reveals a Novel Binding Site Model for Fentanyl at the μ-Opioid Receptor

Author

Govindan Subramanian, M G Paterlini, David M. Ferguson, and Philip S. Portoghese

Subjects

Models, Molecular, Molecular model, Stereochemistry, Molecular Sequence Data, Molecular Conformation, Receptors, Opioid, mu, Ligands, Carfentanil, Structure-Activity Relationship, chemistry.chemical_compound, Receptors, Opioid, delta, Drug Discovery, medicine, Humans, R-30490, Amino Acid Sequence, Binding site, Conformational isomerism, Binding Sites, Chemistry, Receptors, Opioid, kappa, Stereoisomerism, Ligand (biochemistry), Fentanyl, Searching the conformational space for docking, Docking (molecular), Molecular Medicine, medicine.drug

Abstract

The ligand binding modes of a series of fentanyl derivatives are examined using a combination of conformational analysis and molecular docking to the mu-opioid receptor. Condensed-phase molecular dynamics simulations are applied to evaluate potential relationships between ligand conformation and fentanyl substitution and to generate probable "bioactive" structures for the ligand series. Automated docking of the largely populated solution conformers identified a common binding site orientation that places the N-phenethyl group of fentanyl deep in a crevice between transmembrane (TM) helices II and III while the N-phenylpropanamide group projected toward a pocket formed by TM-III, -VI, and -VII domains. An analysis of the binding modes indicates the most potent fentanyl derivatives adopt an extended conformation both in solution and in the bound state, suggesting binding affinity may depend on the conformational preferences of the ligands. The results are consistent with ligand binding data derived from chimeric and mutant receptor studies as well as structure-activity relationship data reported on a wide range of fentanyl analogues. The binding site model is also compared to that of N-phenethylnormorphine. An overlay of the bound conformation of the opiate and cis-3-methylfentanyl shows the N-phenethyl groups occupy equivalent binding domains in the receptor. While the cationic amines of both ligand classes were found docked to an established anchor site (D149 in TM-III), no overlap was observed between the N-phenylpropanamide group and the remaining components of the opiate scaffold. The unique binding mode(s) proposed for the fentanyl series may, in part, explain the difficulties encountered in defining models of recognition at the mu-receptor and suggest opioid receptors may display multiple binding epitopes. Furthermore, the results provide new insight to the design of experiments aimed at understanding the structural basis to the differential selectivities of ligands at the mu-, delta-, and kappa-opioid receptors.

Published

2000

43. The FEMA GRAS Assessment of trans-Anethole Used as a Flavouring Substance

Author

C.S. Weil, Philip S. Portoghese, L.A. Woods, Robert L. Smith, R.A. Ford, I. C. Munro, Jay I. Goodman, John Doull, C.D Lucas, T. B. Adams, Bernard M. Wagner, and P.M. Newberne

Subjects

Metabolite, Cumulative Exposure, Physiology, General Medicine, Toxicology, medicine.disease_cause, Median lethal dose, chemistry.chemical_compound, Pharmacokinetics, chemistry, Toxicity, medicine, Toxicokinetics, Genotoxicity, Anethole, Food Science

Abstract

This publication is the fourth in a series of safety evaluations performed by the Expert Panel of the Flavour and Extract Manufacturers' Association (FEMA). In 1993, the Panel initiated a comprehensive program to re-evaluate the safety of more than 1700 GRAS flavouring substances under conditions of intended use. In this review, scientific data relevant to the safety evaluation of trans-anethole (i.e. 4-methoxypropenylbenzene) as a flavouring substance is critically evaluated by the FEMA Expert Panel. The evaluation uses a mechanism-based approach in which production of the hepatotoxic metabolite anethole epoxide (AE) is used to interpret the pathological changes observed in different species and sexes of laboratory rodents in chronic and subchronic dietary studies. Female Sprague Dawley rats metabolize more trans-anethole to AE than mice or humans and, therefore, are the most conservative model for evaluating the potential for AE-induced hepatotoxicity in humans exposed to trans-anethole from use as a flavouring substance. At low levels of exposure, trans-anethole is efficiently detoxicated in rodents and humans primarily by O-demethylation and omega-oxidation, respectively, while epoxidation is only a minor pathway. At high dose levels in rats, particularly females, a metabolic shift occurs resulting in increased epoxidation and formation of AE. Lower activity of the "fast" acting detoxication enzyme epoxide hydrolase in the female is associated with more pronounced hepatotoxicity compared to that in the male. The continuous intake of high dose levels of trans-anethole (i.e. cumulative exposure) has been shown in dietary studies to induce a continuum of cytotoxicity, cell necrosis and cell proliferation. In chronic dietary studies in rats, hepatotoxicity was observed when the estimated daily hepatic production of AE exceeded 30 mg AE/kg body weight. In female rats, chronic hepatotoxicity and a low incidence of liver tumours were reported at a dietary intake of 550 mg trans-anethole/kg body weight/day. Under these conditions, daily hepatic production of AE exceeded 120 mg/kg body weight. Additionally, neither trans-anethole nor AE show any evidence of genotoxicity. Therefore, the weight of evidence supports the conclusion that hepatocarcinogenic effects in the female rat occur via a non-genotoxic mechanism and are secondary to hepatotoxicity caused by continuous exposure to high hepatocellular concentrations of AE. trans-Anethole was reaffirmed as GRAS (GRASr) based on (1) its low level of flavour intake (54 microg/kg body weight/day); (2) its metabolic detoxication pathway in humans at levels of exposure from use as a flavouring substance; (3) the lack of mutagenic or genotoxic potential; (4) the NOAEL of 120 mg trans-anethole/kg body weight/day in the female rat reported in a 2 + -year study which produces a level of AE (i.e. 22 mg AE/kg body weight/day) at least 10,000 times the level (0.002 mg AE/kg body weight day) produced from the intake of trans-anethole from use as a flavouring substance; and (5) the conclusion that a slight increase in the incidence of hepatocellular tumours in the high dose group (550 mg trans-anethole/kg body weight/day) of female rats was the only significant neoplastic finding in a 2+ -year dietary study. This finding is concluded to be secondary to hepatotoxicity induced by high hepatocellular concentrations of AE generated under conditions of the study. Because trans-anethole undergoes efficient metabolic detoxication in humans at low levels of exposure, the neoplastic effects in rats associated with dose-dependent hepatotoxicity are not indicative of any significant risk to human health from the use of trans-anethole as a flavouring substance.

Published

1999

44. Endomorphin-1 potentiates HIV-1 expression in human brain cell cultures: implication of an atypical μ-opoid receptor

Author

James R. Lokensgard, Phillip K. Peterson, Genya Gekker, Philip S. Portoghese, Chun C. Chao, and Shuxian Hu

Subjects

medicine.medical_specialty, Enkephalin, medicine.drug_class, HIV Core Protein p24, Receptors, Opioid, mu, Pharmacology, Biology, Virus Replication, Pertussis toxin, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Fetus, Opioid receptor, Internal medicine, medicine, Humans, Opioid peptide, Receptor, Cells, Cultured, Cerebral Cortex, Neurons, Endomorphin-1, Enkephalins, Enkephalin, Ala(2)-MePhe(4)-Gly(5), Analgesics, Opioid, Kinetics, DAMGO, Endocrinology, chemistry, HIV-1, Microglia, Neuroglia, Oligopeptides, Endomorphin

Abstract

Endogneous delta and kappa opioid peptides possess a variety of immunomodulatory properties, and kappa-opioid receptor ligands recently were shown to suppress the expression of human immunodeficiency virus type 1 (HIV-1) in microglial cells, the resident macrophages of the brain. To determine whether the newly discovered endogenous mu-opioid receptor ligands endomorphin-1 and -2 would affect HIV-1 replication, these peptides were added to acutely infected brain cell cultures. Endomorphin-1 potentiated viral expression, in a bell-shaped dose-response manner with maximal enhancement approximately equal to 35% at 10(-10) M, in both mixed glial/neuronal cell and purified microglial cell cultures. Endomorphin-1's amplifying effect was blocked by pretreatment of brain cells with either the mu-opioid receptor selective antagonist beta-funaltrexamine or the G protein inhibitor pertussis toxin. However, the classical mu receptor agonists morphine and DAMGO (Tyr-d-Ala-Gly-N-Me-Phe-Gly-ol) had no effect on viral expression or on endomorphin-1's amplifying effect. Taken together, these findings suggest that in this in vitro model of HIV-1 brain infection, endomorphin-1 potentiates viral expression via activation of an atypical mu-selective opioid receptor. They also provide evidence, for the first time, that an endogenous mu-opioid peptide has neuroimmunomodulatory activity.

Published

1999

45. Mutational Evidence for a Common κ Antagonist Binding Pocket in the Wild-Type κ and Mutant μ[K303E] Opioid Receptors

Author

Robert M. Jones, S A Hjorth, Thue W. Schwartz, and Philip S. Portoghese

Subjects

Male, Models, Molecular, Narcotic Antagonists, Guinea Pigs, Molecular Sequence Data, Mutant, Molecular Conformation, Receptors, Opioid, mu, In Vitro Techniques, Binding, Competitive, Guanidines, Mice, chemistry.chemical_compound, Vas Deferens, Ileum, Drug Discovery, medicine, Animals, Amino Acid Sequence, Receptor, Chemistry, Receptors, Opioid, kappa, Antagonist, Wild type, Muscle, Smooth, JDTic, Molecular biology, Naltrexone, Rats, Morphinans, Opioid, Biochemistry, COS Cells, Mutation, Molecular Medicine, Norbinaltorphimine, Kappa, medicine.drug

Published

1998

46. 7-Arylidenenaltrexones as Selective δ1 Opioid Receptor Antagonists

Author

Shigenori Ohkawa and Philip S. Portoghese

Subjects

Male, Tail, medicine.drug_class, Stereochemistry, Narcotic Antagonists, Guinea Pigs, In Vitro Techniques, Ligands, Benzylidene Compounds, Chemical synthesis, Mice, Structure-Activity Relationship, Vas Deferens, Ileum, In vivo, Opioid receptor, Receptors, Opioid, delta, Drug Discovery, medicine, Animals, ED50, Pain Measurement, Mice, Inbred ICR, Narcotic antagonist, Chemistry, Antagonist, Muscle, Smooth, Electric Stimulation, Naltrexone, In vitro, Morphine, Molecular Medicine, Muscle Contraction, medicine.drug

Abstract

A series of 7-arylidinenaltrexones (2a-m) related to the prototypical delta1-selective antagonist, 7-benzylidenenaltrexone 1 (BNTX), have been synthesized in an effort to develop more selective ligands. Testing in smooth muscle preparations revealed that members of the series exhibited varying degrees of selectively for delta receptors, with the o-methoxy (2e) and o-chloro (2j) congeners being most potent and most selective (Ke approximately 0.8 nm). Evaluation of 1, 2e, and 2f sc in mice using the tail-flick procedure indicated that they are selective delta1 opioid receptor antagonists in the lower dose range. At high doses these ligands, including BNTX, exhibited decreased delta1 selectivity due to increases in the ED50 ratios of [D-Ser2,Leu5]enkephalin-Thr6 and morphine. It is concluded that 2e and 2f possess in vivo selectivity similar to that of BNTX, but are less potent as delta1 antagonists.

Published

1998

47. 7-Spirobenzocyclohexyl Derivatives of Naltrexone, Oxymorphone, and Hydromorphone as Selective Opioid Receptor Ligands

Author

Philip S. Portoghese, Xinqin Fang, and Dennis L. Larson

Subjects

Male, Narcotics, Agonist, Stereochemistry, medicine.drug_class, Guinea Pigs, Molecular Conformation, In Vitro Techniques, Ligands, Partial agonist, Mice, Structure-Activity Relationship, Naltrindole, Opioid receptor, Receptors, Opioid, delta, Drug Discovery, medicine, Animals, Hydromorphone, Inverse agonist, Spiro Compounds, Molecular Structure, Oxymorphone, Chemistry, Muscle, Smooth, Receptor antagonist, Electric Stimulation, Naltrexone, Competitive antagonist, Molecular Medicine, Muscle Contraction, medicine.drug

Abstract

On the basis of previous structure-activity studies of the highly potent and selective delta-opioid receptor antagonist naltrindole (1) and the spiroindanyl analogues 2 and 3, we have synthesized epimeric pairs of spirobenzocyclohexyl derivatives of naltrexone, oxymorphone, and hydromorphone (4-9). Pharmacologic evaluation in smooth muscle assays has revealed that the oxymorphone derivatives (6, 7) are delta-selective agonists and possess receptor binding profiles that are consistent with their agonist activity. It is proposed that the spirobenzocyclohexyl group of 6 and 7 orients its benzene moiety orthogonally with respect to the C ring of the opiate in a manner similar to that of the spiroindanyl analogue 3. It is suggested that this orthogonal orientation serves as an "address" to facilitate activation of delta receptors. The finding that the hydromorphone analogues (8, 9) were full mu agonists and exhibited only partial delta agonist activity suggests that the 14-hydroxyl group also contributes to the delta agonist activity. The naltrexone derivatives (4, 5) were mu-selective antagonists and exhibited relatively weak delta antagonist activity. However, the binding data indicated a very high-affinity delta-selective binding profile that was not consistent with the pharmacology. This study illustrates the differential contributions of the delta "address" to agonist and antagonist activity and supports the idea of different recognition sites for interaction of agonist and antagonist ligands with delta-opioid receptors.

Published

1997

48. The FEMA GRAS assessment of furfural used as a flavour ingredient

Author

C.S. Weil, T. B. Adams, John Doull, Robert L. Smith, Bernard M. Wagner, Jay I. Goodman, P.M. Newberne, I. C. Munro, Philip S. Portoghese, L.A. Woods, and R.A. Ford

Subjects

food.ingredient, Metabolic detoxication, business.industry, Food additive, Flavour, Male mice, General Medicine, Toxicology, Furfural, medicine.disease_cause, Ingredient, chemistry.chemical_compound, food, chemistry, Medicine, Food science, business, Flavor, Genotoxicity, Food Science

Abstract

The Expert Panel of the Flavor and Extract Manufacturers' Association (FEMA) has assessed the safety of furfural for its continued use as a flavour ingredient. The safety assessment takes into account the current scientific information on exposure, metabolism, pharmacokinetics, toxicology, carcinogenicity and genotoxicity. Furfural was reaffirmed as GRAS (GRASr) as a flavour ingredient under conditions of intended use based on: (1) its mode of metabolic detoxication in humans; (2) its low level of flavour use compared with higher intake levels as a naturally occurring component of food; (3) the safety factor calculated from results of subchronic and chronic studies, (4) the lack of reactivity with DNA; and (5) the conclusion that the only statistically significant finding in the 2-year NTP bioassays, an increased incidence of hepatocellular adenomas and carcinomas in the high-dose group of male mice, was secondary to pronounced hepatotoxicity. Taken together, these data do not indicate any risk to human health under conditions of use as a flavour ingredient. This evidence of safety is supported by the occurrence of furfural as a natural component of traditional foods, at concentrations in the diet resulting in a 'natural intake' that is at least 100 times higher than the intake of furfural from use as a flavour ingredient.

Published

1997

49. Inhibition of substance P release from spinal cord tissue after pretreatment with capsaicin does not mediate the antinociceptive effect of capsaicin in adult mice

Author

Philip S. Portoghese, Alice A. Larson, Virginia M. Goettl, and Dennis L. Larson

Subjects

Male, Cord, Ratón, Central nervous system, Drug Evaluation, Preclinical, Pain, Neuropeptide, Substance P, Pharmacology, Mice, chemistry.chemical_compound, medicine, Animals, Injections, Spinal, Chemistry, Spinal cord, Perfusion, Anesthesiology and Pain Medicine, medicine.anatomical_structure, Nociception, Spinal Cord, Neurology, Capsaicin, Anesthesia, lipids (amino acids, peptides, and proteins), Neurology (clinical)

Abstract

Substance P (SP) is released from primary afferent fibers in response to nociceptive stimuli. Capsaicin, which produces an initial hyperalgesic response followed by persistent antinociception, also elicits release of SP from primary afferent fibers. Capsaicin pretreatment decreases the content and release of SP from primary afferent fibers. This effect on SP has been hypothesized to mediate the antinociceptive effect of capsaicin. To test this hypothesis, mice were injected intrathecally (i.t.) with antinociceptive doses of capsaicin or SP(1–7) before superfusion of spinal cord tissue with 3 μ M capsaicin 24, 48, 96 or 168 h later. N-terminal metabolic fragments of SP that accumulate after capsaicin-induced SP release and are involved in the antinociceptive effect of capsaicin, were also tested. Like capsaicin SP(1–3), SP(1–4) and SP(1–7) were each antinociceptive when injected 24 h before nociceptive testing. However, at this time there was no decrease in capsaicin-evoked release of SP in tissue from capsaicin- and SP(1–7)-pretreated animals compared to those injected with vehicle. In contrast, capsaicin-evoked SP release decreased significantly in tissue from mice pretreated with capsaicin or SP(1–7) 48 h prior to testing. d -Substance P(1–7), which prevents antinociception, blocked capsaicin- and SP(1–7)-induced decreases in SP release, indicating that these effects are mediated by SP N-terminal activity. Total spinal cord content of SP did not differ amongst treatment groups. These data indicate that antinociception does not appear to depend on decreases in SP release or content as antinociception precedes decreases in SP release.

Published

1997

50. Pyrrolomorphinans as δ Opioid Receptor Antagonists. The Role of Steric Hindrance in Conferring Selectivity

Author

F. Farouz-Grant and Philip S. Portoghese

Subjects

Male, Steric effects, medicine.drug_class, Stereochemistry, Guinea Pigs, Stereoisomerism, Ethylketocyclazocine, κ-opioid receptor, δ-opioid receptor, Mice, Opioid receptor, Receptors, Opioid, delta, Drug Discovery, medicine, Animals, Pyrroles, Morphine, Chemistry, Antagonist, Muscle, Smooth, Enkephalin, Leucine-2-Alanine, Electric Stimulation, Models, Chemical, Morphinans, Molecular Medicine, Pharmacophore, Selectivity

Abstract

A series of 2',3'-disubstituted pyrrolomorphinans (5a-i) were synthesized to determine the role of steric hindrance at mu and kappa receptors in promoting delta opioid receptor antagonist selectivity. In smooth muscle preparations, five members of the series (5a-c,e,f) possessed Ke values in the range 2-15 nM and were delta selective. Since the unsubstituted analogue 4 possessed delta antagonist potency of similar magnitude, but was not delta selective, it is suggested that the 2',3'-substitution confers delta selectivity by hindering the interaction of the pharmacophore at mu and kappa receptors, while not affecting delta receptors.

Published

1997